UNITED STATES
                      SECURITIES AND EXCHANGE COMMISSION
                            WASHINGTON, D.C. 20549
                            -----------------------
                                   FORM 10-K

               Annual Report Pursuant to Section 13 or 15(d) of
                      The Securities Exchange Act of 1934
                            -----------------------
                                                Commission
            For the fiscal year ended JUNE 30, 1995File Number 0-12957


                                 ENZON, INC.
            (Exact name of registrant as specified in its charter)

                        DELAWARE               22-2372868
            (State or other jurisdiction of(I.R.S. Employer
            incorporation or organization)Identification No.)

            20 KINGSBRIDGE ROAD, PISCATAWAY, NEW JERSEY     08854
            (Address of principal executive offices)   (Zip Code)

            Registrant's telephone number, including area code: (908) 980-4500

            Securities registered pursuant to Section 12(b) of the Act: NONE

            Securities registered pursuant to Section 12(g) of the Act:

                         COMMON STOCK, $.01 PAR VALUE
                               (Title of class)

      Indicate by check mark whether the registrant (1) has filed  all  reports
required  to be filed by Section 13 or 15(d) of the Securities Exchange Act  of
1934 during  the  preceding  12  months  (or  for  such shorter period that the
registrant was required to file such reports), and (2) has been subject to such
filing requirements for the past 90 days.   Yes  X    No

      Indicate  by check mark if disclosure of delinquent  filers  pursuant  to
item 405 of Regulation  S-K is not contained herein, and will not be contained,
to the best of registrant's  knowledge,  in  definitive  proxy  or  information
statements  incorporated  by  reference  in  Part III of this Form 10-K or  any
amendment to this Form 10-K.

      The aggregate market value of the Common Stock, par value $.01 per share,
held by non-affiliates based upon the reported  last  sale  price of the Common
Stock on September 15, 1995 was approximately $96,025,000.  There  is no market
for  the Series A Cumulative Convertible Preferred Stock, the only other  class
of voting stock.

      As  of  September 15, 1995, there were 26,328,874 shares of Common Stock,
par value $.01 per share, outstanding.

      The Index to Exhibits appears on page 25.

                      DOCUMENTS INCORPORATED BY REFERENCE

      The registrant's  definitive  Proxy  Statement  for the Annual Meeting of
Stockholders scheduled to be held on December 5, 1995,  to  be  filed  with the
Commission  not  later that 120 days after the close of the registrant's fiscal
year, has been incorporated  by  reference,  in whole or in part, into Part III
Items 10, 11, 12 and 13 of this Annual Report on Form 10-K.


                                  ENZON, INC.

                         1995 Form 10-K Annual Report

                               TABLE OF CONTENTS

                                                                   PAGE

                                    PART I
Item 1.   Business                                               3
Item 2.   Properties                                            19
Item 3.   Legal Proceedings                                     19
Item 4.   Submission of Matters to a Vote of
      Security Holders                                      19

                                    PART II

Item 5.   Market for the Registrant's Common Equity and
            Related Stockholder Matters                         20
Item 6.   Selected Financial Data                               21
Item 7.   Management's Discussion and Analysis of Financial
            Condition and Results of Operations                 21
Item 8.   Financial Statements and Supplementary Data           24
Item 9.   Changes in and Disagreements With Accountants
            on Accounting and Financial Disclosure              24

                                   PART III

Item 10.  Directors and Executive Officers of the Registrant24
Item 11.  Executive Compensation                                24
Item 12.  Security Ownership of Certain Beneficial Owners
            and Management                                      24
Item 13.  Certain Relationships and Related Transactions        24

                                    PART IV

Item 14.  Exhibits, Financial Statement Schedules and
            Reports on Form 8-K                                 24




      The following trademarks and service marks  appear in this Annual Report:
      ADAGEN and ONCASPAR are registered trademarks  of Enzon, Inc.;  PEGNOLOGY
      is a registered service mark of Enzon, Inc.; SCA  is a trademark of Enzon
      Labs Inc.; DISMUTEC is a trademark of Sanofi Winthrop,  Inc.; Elspar is a
      registered  trademark  of  Merck  &  Co.,  Inc;  Erwinase is a registered
      trademark of Porton Products Limited; INTRON A is  a registered trademark
      of  Schering  Corporation; BABS is a trademark of Creative  BioMolecules,
      Inc.; and CEREDASE is a trademark of Genzyme Corporation.


                                    PART I

ITEM 1. BUSINESS

OVERVIEW

      Enzon, Inc. ("Enzon"  or  the  "Company")  is a biopharmaceutical company
that   develops,   manufactures   and   markets   enhanced   therapeutics   for
life-threatening   diseases   through   the   application  of  its  proprietary
technologies,   PEG   Modification   or  the  PEG  Process   and   Single-Chain
Antigen-Binding  (SCA)  proteins.  The Company  is  primarily  engaged  in  the
research, development and  commercialization of its proprietary technologies in
the areas of  blood substitutes, genetic diseases and oncology.

      The Company has received  marketing  approval from the United States Food
and Drug Administration ("FDA") for two of its products: (i) ONCASPAR, approved
in February 1994 for the indication of acute  lymphoblastic leukemia ("ALL") in
patients  who are hypersensitive to native forms  of  L-asparaginase  and  (ii)
ADAGEN, the  first  successful application of enzyme replacement therapy for an
inherited disease, approved  in  March  1990  to  treat  a  rare form of Severe
Combined Immunodeficiency Disease ("SCID"), commonly known as  the  Bubble  Boy
Disease.

      The   Company   manufactures  both  ADAGEN  and  ONCASPAR  in  its  South
Plainfield, New Jersey  facility  and  markets  ADAGEN  on  a  worldwide basis.
ONCASPAR  is marketed in the U.S. by Rhone-Poulenc Rorer Pharmaceuticals,  Inc.
("RPR").  The  Company  received $6,000,000 from RPR related to the granting of
this license (of which $500,000  and $5,500,000 were paid to the Company during
the  fiscal  years ended June 30, 1995  and  1994,  respectively).   Under  the
license, which  was  amended  in  January 1995, the Company is also entitled to
royalties on the sales of ONCASPAR  in  the U.S. by RPR of 10% to 23.5% in 1995
and 23.5% to 43.5%, thereafter, based on  the  sales level of ONCASPAR.  During
1995,  RPR  paid the Company $3,500,000 in advance  royalties.   Royalties  due
under the RPR  agreement  will  be offset against a credit of $5,970,000, which
represents the royalty advance plus  reimbursement  of  certain amounts due RPR
under  the  original  agreement  and  interest expense.  The Company  has  also
granted exclusive licenses to sell ONCASPAR  in  Canada  and  Mexico  to RPR in
exchange  for  royalty  payments  on  future  sales.   The Company is currently
pursuing  additional  licenses  for marketing and distribution  rights  outside
North America.  During November 1994,  ONCASPAR was approved in Germany for use
in patients with ALL who are hypersensitive to natural forms of L-asparaginase.

      ONCASPAR is the enzyme L-asparaginase  modified  by  the  PEG Process and
ADAGEN is the enzyme adenosine deaminase modified by the PEG Process.   The PEG
Process involves chemically attaching polyethylene glycol ("PEG"), a relatively
non-reactive   and   non-toxic   polymer,   to   proteins   and  certain  other
pharmaceuticals   for  the  purpose  of  enhancing  their  therapeutic   value.
Attachment  of  PEG  helps  to  disguise  the  proteins  and  to  reduce  their
recognition  by  the  immune   system,  thereby  generally  lowering  potential
immunogenicity.  Both the increased  molecular  size  and  lower immunogenicity
result in extended circulating blood life, in some cases from minutes to days.

      In addition to its approved products, the Company is conducting  research
and  developing  additional  drugs.  In the blood substitutes area, the Company
has undertaken the development  of a hemoglobin based oxygen carrier, utilizing
the protein hemoglobin modified by the PEG Process. In addition to its use as a
blood  substitute,  the  Company's  product   PEG-hemoglobin,   may  act  as  a
radiosensitizer in cancer therapy.  Enzon has chosen to base PEG-hemoglobin  on
bovine  hemoglobin,  due  to  its superior oxygen-carrying properties, relative
stability, availability and low  cost.   The  Company is currently conducting a
Phase  I  clinical  trial  in  healthy  volunteers and  has  administered  PEG-
hemoglobin  to  28  subjects up to a dose of  approximately  45  grams  or  the
equivalent of approximately 1.5 units of whole blood.  The Company is compiling
the results of this trial  for  submission  to  the  FDA.  The Company plans to
conduct future clinical trials utilizing PEG-hemoglobin  in  patients receiving
radiation  treatment  for  solid  hypoxic  tumors  and  as  a  blood substitute
(resuscitation  fluid)  for  trauma  patients.   The Company is discussing  the
protocols  for these trials with the FDA.  The Company  currently  manufactures
and plans to  manufacture  PEG-hemoglobin  for  future  trials in a pilot plant
facility located in South Plainfield, New Jersey.

      In  the  area  of  genetic  diseases,  the Company's lead  product  under
development is a PEG-modified version of the enzyme glucocerebrosidase to treat
Gaucher  disease,  a  genetic  disorder  that results  in  the  lack  of  beta-
glucocerebrosidase, an enzyme instrumental  in  the  breakdown  and disposal of
complex fatty substances in the bloodstream.  These substances then  accumulate
in  the  spleen,  liver  and  bone marrow, resulting in anemia, weakened bones,
enlargement of the spleen and liver  and  sometimes  early death.  An estimated
15,000 people suffer from Gaucher disease in the United  States,  of whom 2,000
to 3,000 require medical attention.  During September 1994, the Company began a
Phase  I  clinical  trial  in  Gaucher  patients.  Currently, two patients  are
enrolled in this trial and additional patients are anticipated to be added when
clinical trial material becomes available.

      The  Company  has  several products under  development  in  the  area  of
oncology which are all in  the  early  research  stage.  These products include
PEG-modified anti-cancer compounds and a novel chemical compound.

      The  Company  is  pursuing  a  dual  strategy  for   commercializing  its
proprietary  technologies.   In  addition  to  developing,  manufacturing   and
marketing  the  Company's  proprietary  products,  the  Company has established
strategic  alliances  in which Enzon licenses its proprietary  technologies  in
exchange for milestone payments, manufacturing revenues and/or royalties.

      The Company licensed  exclusive  worldwide  marketing  rights  to  Sanofi
Winthrop  Inc. ("Sanofi"), formerly Sterling Winthrop, Inc., for PEG-Superoxide
dismutase  ("PEG-SOD"),  which  is  the  enzyme  superoxide  dismutase  ("SOD")
modified by  the PEG Process. SOD destroys oxygen free radicals that may damage
tissue  during   reperfusion   associated  with  myocardial  infarction,  organ
transplant and trauma.  Generally,  Enzon  will  be  entitled to 40% of the net
profits from sales of PEG-SOD in the United States during the life of the basic
U.S. PEG patent covering this product, with agreed-upon limits on the amount of
expenses that can be deducted by Sanofi from revenues  before  calculating  the
profit split.  Sanofi is presently developing PEG-SOD, which it has trademarked
as DISMUTEC, for closed head trauma.  Sanofi has advised the Company that it is
currently  conducting an expanded Phase III clinical trial on PEG-SOD, which is
expected to  be completed during the fourth quarter of 1995.  A smaller, double
blind, Phase III  study  with  approximately  460  patients has been completed.
This study showed that patients receiving DISMUTEC showed  18% and 16% relative
improvement in favorable neurological outcomes compared to patients receiving a
placebo,  three  and  six months after injury, respectively. Published  sources
indicate that the FDA has  granted PEG-SOD "fast track" status in the FDA's new
drug approval process.  The  Company and Research Corporation Technologies Inc.
("RCT") signed agreements seeking  to  extend  the PEG patent for this product.
See "Research Corporation License Agreements".

      The Company is also developing a PEG version  of  a  Schering Corporation
("Schering") product, INTRON A (interferon alfa 2b).  During  the  fiscal  year
ended June 30, 1995, the Company amended its agreement with Schering and agreed
to  transfer  proprietary  know-how  and  manufacturing  rights to Schering for
$3,000,000, of which $2,000,000 was received during the fiscal  year ended June
30,  1995.   The Company also sold to Schering, 847,000 shares of unregistered,
newly issued Common  Stock  for  gross  proceeds of $2,000,000.  The Company is
also entitled to additional payments of approximately  $5,550,000,  subject  to
the  achievement  of  certain  milestones  in  the  product's  development, and
royalties  on  worldwide  sales of PEG INTRON A, if any.  The Company  has  the
option, upon FDA approval,  to  be  Schering's  exclusive  manufacturer  of PEG
INTRON A for the U.S. market.

      The  Company  has  an extensive licensing program for its SCA technology.
SCA proteins are genetically  engineered  proteins  designed  to  overcome  the
problems   hampering   the  diagnostic  and  therapeutic  use  of  conventional
monoclonal antibodies.   Pre-clinical  studies  have  shown  that  SCA proteins
target   and   penetrate  tumors  more  readily  than  conventional  monoclonal
antibodies.  Currently,  there are five SCA proteins in Phase I clinical trials
by various organizations,  including  a  product developed by the Company, SCA-
CC49.  The Company believes these organizations  will  have to obtain a license
from the Company under its SCA patents to commercialize  these  products.   See
"Patents".   The  Company  believes  that  SCA  proteins  may  be useful in the
development of therapeutics in the area of oncology.

      The Company has granted SCA licenses to six companies, including Bristol-
Myers Squibb, Inc. ("Bristol-Myers"), Baxter Healthcare Corporation  ("Baxter")
and  Eli  Lilly  &  Co.  ("Eli  Lilly").   These licenses generally provide for
upfront payments, milestone payments and royalties  on  sales  of  FDA approved
products.

PRODUCTS ON THE MARKET

      The  Company  currently  has  two  products  on the market, ONCASPAR  and
ADAGEN.  The Company received marketing approval from  the  FDA for ONCASPAR in
February 1994 and for ADAGEN in March 1990.

ONCASPAR

      ONCASPAR, the enzyme L-asparaginase modified by the PEG  Process, is used
in conjunction with other chemotherapeutics to treat patients with  ALL who are
hypersensitive (allergic) to native (unmodified) forms of L-asparaginase.

      L-asparaginase  is an enzyme which depletes the amino acid asparagine,  a
non-essential amino acid  upon  which  certain leukemic cells are dependent for
survival. Accordingly, the depletion of  plasma  asparagine  levels selectively
starves  these  leukemic  cells.  L-asparaginase  is  a  component of  standard
pediatric  ALL  remission  induction  therapies.  Unmodified L-asparaginase  is
currently   marketed   as  Elspar.   Erwinase,  another  form   of   unmodified
L-asparaginase, is also  available  in the United States on a compassionate use
basis, but is not FDA approved.

      The therapeutic value of unmodified  L-asparaginase  is  limited  by  two
inherent features of the enzyme. First, its short half-life in blood (less than
1.5  days)  requires every-other-day injections, causing significant discomfort
and inconvenience  to  patients.  Secondly, the enzyme's non-human source makes
it inherently immunogenic, resulting in a high incidence of allergic reactions,
some  of  which  may  be  severe,   necessitating  the  discontinuance  of  the
L-asparaginase therapy.

      Through  PEG Modification, Enzon  believes  ONCASPAR  offers  significant
therapeutic advantages  over  unmodified L-asparaginase. Namely, ONCASPAR has a
significantly increased half-life  in  blood (greater than five days), allowing
every-other-week administration, making its use more tolerable to patients than
unmodified L-asparaginase. PEG Modification also disguises the enzyme's foreign
nature, generally reducing its immunogenicity,  and  accordingly, the incidence
of allergic reactions.

      ONCASPAR was launched in the United States by RPR during March 1994.  The
Company has granted RPR an exclusive license ("the RPR  License  Agreement") in
the United States to sell ONCASPAR, and any other PEG-asparaginase product (the
"Product") developed by Enzon or RPR during the term of the License  Agreement.
Under  this  agreement,  Enzon  is  entitled  to  licensing  payments  totaling
$6,000,000, of which $500,000 and $5,500,000 were paid during the fiscal  years
ended  June  30, 1995 and 1994, respectively.  During January 1995, the Company
amended the RPR  License  Agreement.   Under the amended RPR License Agreement,
Enzon will earn a base royalty of 10% for the year ending December 31, 1995 and
23.5%  thereafter, until 2008, on net sales  of  ONCASPAR  up  to  agreed  upon
amounts,  as  opposed  to  50%  of  net  profits  under the original agreement.
Additionally,  Enzon will earn a super royalty of 23.5%  for  the  year  ending
December 31, 1995  and  43.5%  thereafter, until 2008, on net sales of ONCASPAR
which  exceed the agreed upon amounts,  with  the  limitation  that  the  total
royalties  earned  for  any  such  year shall not exceed 33% of net sales.  The
revision eliminates RPR's requirement  to  make  certain  minimum  advertising,
promotional  and  clinical  expenditures.   Future decisions regarding clinical
development will be at RPR's discretion.  The  amended  RPR  License  Agreement
also  provides  for  a  payment  of  $3,500,000 in advance royalties, which was
received in January 1995.

      The payment of base royalties to  Enzon  under  the  amended  RPR License
Agreement  will  be  offset  by  a  credit of $5,970,000, which represents  the
royalty advance plus reimbursement of  certain  amounts  due  to  RPR under the
original RPR License Agreement and interest expense.  Super royalties  will  be
paid  to  the Company when earned.  The royalty advance is shown as a long term
liability,  with the corresponding current portion included in accrued expenses
on the Consolidated  Balance  Sheet  as  of June 30, 1995.  The royalty advance
will be reduced as base royalties are recognized under the agreement.

      The amended RPR License Agreement prohibits  RPR from selling a competing
PEG-asparaginase  product  anywhere  in  the  world during  the  term  of  such
agreement  and for five years thereafter.  The amended  RPR  License  Agreement
terminates in  December  2008, subject to early termination by either party due
to a default by the other  or  by RPR at any time on one year's prior notice to
Enzon.  Upon any termination all rights under the amended RPR License Agreement
revert to Enzon.

      The Company has also granted  exclusive  licenses  to  sell  ONCASPAR  in
Canada and Mexico to RPR.  These agreements provide for RPR to obtain marketing
approval  of  ONCASPAR  in  Canada  and  Mexico  and for the Company to receive
royalties on sales of ONCASPAR in these countries,  if  any.   The  Company  is
currently  pursuing  other  licenses  for marketing and distribution rights for
ONCASPAR outside North America.  A separate  supply agreement with RPR requires
RPR to purchase from Enzon all of RPR's requirements  for the Product for sales
in North America.

      In  November  1994,  the  Company  received  approval  in   Germany   for
therapeutic  use  of  ONCASPAR  in  patients with ALL who are hypersensitive to
natural forms of L-asparaginase.  The Company is currently not selling ONCASPAR
in Germany.  The Company is pursuing  marketing  and distribution agreements in
countries outside of North America, including Germany.

ADAGEN

      ADAGEN, the Company's first FDA approved product, is currently being used
to treat 43 patients in six countries.  ADAGEN represents  the first successful
application  of enzyme replacement therapy for an inherited disease.   ADAGEN's
Orphan Drug designation  under  the  Orphan  Drug Act provides the Company with
marketing exclusivity in the United States through March 1997.

      ADAGEN, the enzyme adenosine deaminase ("ADA")  modified  through the PEG
Process,  was  developed  by  the  Company  for the treatment of ADA deficiency
associated with SCID.  Commonly known as the  "bubble  boy"  disease, SCID is a
congenital   disease  that  results  in  children  being  born  without   fully
functioning immune  systems,  leaving  them  susceptible  to  a  wide  range of
infectious  diseases.   Injections  of  unmodified  ADA  would not be effective
because of its short circulating blood life (less than thirty  minutes) and the
potential for immunogenic reactions to a bovine-sourced enzyme.  The attachment
of PEG to ADA allows ADA to achieve its full therapeutic effect  by  increasing
its circulating life and masking the ADA to avoid immunogenic reactions.

      ADAGEN  is  being  marketed  on  a worldwide basis and sold in the United
States by the Company.  Distribution of  ADAGEN in Europe is being handled by a
European  firm.   Enzon  believes  many newborns  with  ADA-deficient  SCID  go
undiagnosed, and is therefore focusing  its marketing efforts for ADAGEN on new
patient identification.  Its marketing efforts  include  targeted  advertising,
educational   presentations   and  publications  designed  to  encourage  early
diagnosis and subsequent ADAGEN treatment.

      Sales of ADAGEN for the fiscal  years  ended June 30, 1995, 1994 and 1993
were $8,305,000, $7,601,000, and $5,788,000, respectively.  Sales of ADAGEN are
expected  to  continue  to  be  limited  due to the  small  patient  population
worldwide.

RESEARCH AND DEVELOPMENT

      The Company's primary source of new products is its internal research and
development activities. Research and development  expenses for the fiscal years
ended June 30, 1995, 1994 and 1993 were approximately $12,084,000, $17,665,000,
and $17,710,000, respectively.  During fiscal 1995,  research  and  development
expenses  were  divided  as  follows:  17%  for research; 42% for clinical  and
regulatory affairs; and 41% for pre-clinical activities.

      The  Company's research and development  activities  during  fiscal  1995
concentrated   primarily   on   the  continued  development  of  two  products,
PEG-hemoglobin   and   PEG-glucocerebrosidase.     These   activities   related
principally to Phase I clinical testing, scale up and  process  development and
pre-clinical testing.  Research and development activities also included  early
stage  development  of  several  oncology  products  and  enhancements  to  the
Company's proprietary technologies.

TECHNOLOGIES AND CAPABILITIES

PEG-MODIFICATION

      Enzon's  proprietary  technology,  PEG  Modification  or the PEG Process,
involves   chemically   attaching   PEG   to   proteins   and   certain   other
pharmaceuticals.   PEG  is  a  relatively  non-reactive  and  non-toxic polymer
typically used in many food and drug products.  Attachment of PEG disguises the
proteins, and reduces their recognition by the immune system, thereby generally
lowering potential immunogenicity and extending their circulating life, in some
cases from minutes to days.  Enzon believes that proteins modified  by  the PEG
Process  may  offer  significant advantages over their unmodified forms.  These
advantages include: (i)  extended  circulating  life, (ii) reduced incidence of
allergic  reactions,  (iii) reduced dosages with corresponding  lower  toxicity
without diminished efficacy,  (iv)  increased  drug stability, and (v) enhanced
drug solubility.  Modification of proteins with  the  PEG  Process often causes
these  proteins  to  have  characteristics  which  significantly improve  their
therapeutic   performance,   and   in  some  cases  enables  proteins   to   be
therapeutically effective which, in  their  unmodified forms, have proven to be
unacceptably toxic or non-efficacious.

      The Company and its senior scientists have developed proprietary know-how
which  significantly  improves  the PEG Process  over  that  described  in  the
original patent covering this technology.   This  proprietary  know-how enables
the Company to tailor the PEG Process in order to produce the targeted  results
for  the  particular  substance  being modified.  This know-how includes, among
other things, proprietary linkers for the attachment of PEG to the protein, the
selection of the appropriate attachment  sites  on  the surface of the protein,
and the amount and type of PEG used.  The Company has filed patent applications
and has received patents for numerous improvements to  the  PEG  Process.   See
"Patents".

SINGLE-CHAIN ANTIGEN-BINDING (SCA) PROTEINS

      Enzon's  proprietary  SCA  proteins  are  genetically engineered proteins
designed  to  overcome the problems associated with  the  therapeutic  uses  of
monoclonal antibodies.   SCA proteins have the binding specificity and affinity
of monoclonal antibodies,  but  Enzon believes that SCA proteins offer at least
five  significant  advantages  over  conventional  monoclonal  antibodies:  (i)
greater tumor penetration for cancer  imaging  and  therapy, (ii) more specific
localization to target sites in the body, (iii) a significant  decrease  in the
immunogenic problems associated with monoclonals due to the SCA protein's small
size  and  rapid  clearance  from the body, (iv) easier and more cost effective
scale-up for manufacturing, and (v) enhanced screening capabilities which allow
for  the  testing  of  SCA proteins  for  desired  specificities  using  simple
screening methods.

      Enzon's  research  and   development  capabilities  for  engineering  SCA
proteins include: (i) using computer  modeling  to  design  linker  peptides to
connect  the  two protein chains, and (ii) linking the two protein chains  that
make up the antigen-binding  region  of  a  natural antibody with such designed
peptides, producing a single-chain protein that  preserves  the  structural and
functional  integrity  of the binding region.  The resulting protein  chain  is
approximately one-sixth  the size of a natural antibody.  The SCA protein has a
binding specificity and affinity  nearly  identical to that of a single binding
region of the monoclonal antibody from which the SCA protein was derived.

      The binding specificity of SCA proteins has been demonstrated through the
preparation and in vitro testing of more than a dozen different SCA proteins by
Enzon.  In addition, the Company, in collaboration  with  Dr. Jeffrey Schlom of
the Laboratory of Tumor Immunology and Biology at the National Cancer Institute
("NCI"), has shown in published pre-clinical studies that SCA proteins localize
to specific tumors and rapidly penetrate the tumors.

      The  Company  intends  to  commercialize  its SCA protein  technology  by
licensing the technology to other companies.  To  date, the Company has granted
SCA licenses to six companies, including Bristol-Myers,  Baxter  and Eli Lilly.
These  licenses generally provide for upfront payments, milestone payments  and
royalties  on  sales  of  FDA  approved products.  See "Strategic Alliances and
License Agreements".

      Currently, there are five  SCA  proteins  in  Phase  I clinical trials by
various organizations, including a product developed by the  Company, SCA-CC49.
The Company believes these organizations will have to obtain a license from the
Company to commercialize these products.

PRODUCTS UNDER DEVELOPMENT

      Enzon's development of its proprietary products is focused in three major
areas: (i) blood substitutes,  (ii) genetic diseases,  and  (iii) oncology.

BLOOD SUBSTITUTES

HEMOGLOBIN BASED OXYGEN CARRIER

      The  main  function  of  human  blood is to transport and deliver  oxygen
throughout the body.  Between 12 and 14  million  units  of donated human blood
are transfused to patients suffering from acute blood loss  each  year  in  the
United States.  Without this source, many surgical and trauma patients would be
at high risk for mortality.  Also, the use of donated blood, while effective in
supplying  oxygen  to  patients  suffering  from  acute blood loss, has several
limitations: (i) donated blood spoils in an hour or  two  if  not refrigerated,
(ii)  transfused  blood can only be used in patients having a compatible  blood
type,  and  (iii) donor  blood  can  cause  mortal  risk  of  its  own  due  to
contamination  by  blood  borne  diseases which are difficult to detect and for
which there may be a delay between  exposure  and  detectability.  Such viruses
include hepatitis and Human Immunodeficiency Virus ("HIV")  which  causes AIDS.
Delays  in treatment of patients resulting from the need to type donated  blood
before transfusion, limited supply of certain types of blood and the relatively
short shelf  life  of donor blood, limits the availability of donated blood for
treatment of patients with acute blood loss.

      Currently, there  is  no  commercially  available  blood  substitute that
addresses  these  problems.   Products  that  could  be  used  as  adjuncts  or
alternatives  to the transfusion of red blood cells obtained from human  donors
have been under  development  for  many  years.  One developmental approach has
utilized hemoglobin derived from red blood  cells.   Hemoglobin  is the oxygen-
carrying component of the red blood cell.

      Enzon  has  undertaken  the  development  of PEG-hemoglobin, a hemoglobin
based oxygen carrier, which the Company believes  can be developed with product
specifications consistent with FDA guidelines and which  can  be commercialized
on  a  cost  effective  basis.   The  Company's  goals for its blood substitute
program include the development of a product which  (i)  sufficiently binds and
delivers  oxygen  in  required  quantities during, or after, blood  loss,  (ii)
achieves FDA standards of purity  and  homogeneity,  (iii) is safe, and (iv) is
cost effective and convenient to use.

      Hemoglobin  by  itself  is very toxic and has a short  circulation  life.
Many of the undesirable effects  historically  associated with hemoglobin based
blood  substitutes,  such  as  vasoconstriction,  kidney   dysfunction,   liver
dysfunction  and  gastrointestinal  distress  are a result of these properties.
The Company believes that hemoglobin, modified  through  its  PEG Process, will
overcome  the well-documented problems of toxicity and short circulating  blood
life associated with other forms of blood substitutes that have been developed.
Enzon has chosen  to  develop PEG-hemoglobin utilizing bovine hemoglobin, based
upon its superior oxygen-carrying  properties, relative stability, availability
and low cost.

      In addition to PEG-hemoglobin's potential usefulness as an oxygen carrier
in such indications as trauma and elective surgery, recent pre-clinical studies
suggest that PEG-hemoglobin may act as a radiosensitizer in cancer therapy.  In
1994, the FDA published a paper entitled "Points to Consider in the Development
of a Hemoglobin-Based Oxygen Carrier"  that  discusses  the problems associated
with  determining  clinical  endpoints  that  will demonstrate  efficacy  of  a
hemoglobin-based   oxygen   carrier.   The  paper  recommends   the   following
indications   that   will   simplify   such   endpoints:   regional   perfusion
(radiosensitization), acute hemorrhagic  shock  and perioperative applications.
The endpoint used for radiosensitization (regional  perfusion) will be the same
as the endpoints established for cytotoxic agents, a  reduction  in tumor size.
Approximately 800,000 patients in the U.S. each year are diagnosed  with  solid
hypoxic tumors, such as head and neck, lung, mammary, colon, prostate, bladder,
fibrous  histiocytoma,  brain  metastases  and  glioma.   Pre-clinical  testing
suggests  that  multiple doses of PEG-hemoglobin have delivered oxygen to solid
hypoxic tumors, thereby enhancing the effects of radiotherapy (radiation) which
significantly decreased the size of the tumor.

      The Company  is  currently conducting a Phase I clinical trial in healthy
volunteers and has administered  PEG-hemoglobin  to 28 subjects up to a dose of
approximately 45 grams or the equivalent of approximately  1.5  units  of whole
blood.  The Company is compiling the results of this trial.  The Company  plans
to conduct future clinical trials in patients receiving radiation treatment for
solid  hypoxic tumors and as a blood substitute (resuscitation fluid) in trauma
patients.   The  Company is currently discussing the protocols for these trials
with  the FDA.  The  Company  anticipates  that  patients  receiving  radiation
treatment  will receive multiple doses of PEG-hemoglobin of less than 1.5 units
per dose over the course of treatment.

      Successful  commercialization  of  an  artificial  blood  substitute will
require an adequate supply of raw material.  The Company's main competitors  in
the  development  of  a hemoglobin based oxygen carrier utilize either outdated
human blood or recombinant  hemoglobin  produced  through  fermentation.   Each
source  of  hemoglobin  has  various  problems  associated with it.  The use of
outdated human donor blood relies on a hemoglobin source which is at risk, both
in terms of safety and supply availability.  In the case of non-human or mutant
(genetically  engineered)  hemoglobin,  there  is  a  risk   of   eliciting  an
immunogenic  or  allergic  response to what the body considers to be a  foreign
protein.  The Company believes  that  the use of genetic engineering techniques
to  produce  a  safe  hemoglobin  in commercial  quantities  will  require  the
development of manufacturing capabilities which to date have generally not been
demonstrated.  The Company's product  utilizes  bovine  (cow) hemoglobin, which
can be obtained at relatively low cost.  The Company currently  obtains its raw
hemoglobin from a small herd of cattle which is isolated from other animals and
receives  constant  veterinary care and testing, which should insure  that  the
herd remains disease  free.   In  addition  to keeping the herd virus free, the
Company's  manufacturing  process  provides  or  will  provide  virus  removal,
inactivation and filtration steps.  Enzon believes  it can supply the potential
market demand for PEG-hemoglobin through a relatively small number of animals.

      In  addition  to  the benefit of eliminating the possibility  of  disease
transmissions,  the  Company   believes   that   PEG-hemoglobin  overcomes  the
limitation  of  donor  blood  with regard to compatibility.   The  benefits  of
universal compatibility include  the  ability  to  use  PEG-hemoglobin before a
patient  blood  type is determined, which eliminates problems  associated  with
mistakes in blood typing, which could result in mortality.  PEG-hemoglobin also
has  advantages  over   donated   blood   in   shelf   life.   PEG-hemoglobin's
unrefrigerated  shelf  life  (25c)  is  approximately  seven  days,  as
compared to hours for whole blood.  PEG-hemoglobin also has a frozen shelf life
(-20c) in excess of 18 months and is ready  to  use  immediately  after
thawing.

      The  Company  uses  a  proprietary  process  for  the  separation  of and
purification  of  the  bovine  hemoglobin  and  the  attachment  of  PEG to the
hemoglobin molecule.
      Enzon   presently  produces  PEG-hemoglobin  in  a  pilot  plant  at  its
facilities in South  Plainfield,  New Jersey.  This plant is expected to supply
the  quantities  of  PEG-hemoglobin  needed   for   all  ongoing  research  and
development through Phase II clinical trials.

      The Company estimates that development of a PEG-hemoglobin  product  will
take  several  years and require substantial additional funds.  There can be no
assurance that a  PEG-hemoglobin  product  can  be  successfully  developed and
brought   to  market.   Due  to  the  significant  costs  associated  with  the
development  and  marketing  of  a  blood  substitute  product,  the Company is
currently  exploring  potential  collaborative  arrangements with one  or  more
established pharmaceutical companies.  To date, no  such  agreements  have been
concluded  and  there  can  be  no  assurance  that any such agreements will be
consummated.  Furthermore, there can be no assurance of market acceptability of
a hemoglobin-based oxygen carrier produced from bovine hemoglobin.

GENETIC DISEASES

      There  are diseases which are due solely to  genetic  defects  or  inborn
errors of metabolism  resulting  in  certain enzyme deficiencies, such as SCID,
Gaucher disease and Fabry's disease.  The Company believes that the PEG Process
can  be  used  to successfully replace essential  enzymes  which  patients  are
lacking as a result of such genetic disorders.  The PEG Process has made enzyme
replacement therapy a viable option for the treatment of genetic diseases.

PEG-GLUCOCEREBROSIDASE

      The Company is developing a treatment for Gaucher disease by applying the
PEG  Process  to a  recombinant  form  of  glucocerebrosidase  licensed  on  an
exclusive basis  from  the  National  Institutes  of  Health  ("NIH").  Gaucher
disease   is   a   genetic   disorder   that  results  in  the  lack  of  beta-
glucocerebrosidase, an enzyme instrumental  in  the  breakdown  and disposal of
complex fatty substances in the bloodstream.  These substances then  accumulate
in  the  spleen,  liver  and  bone marrow, resulting in anemia, weakened bones,
enlargement of the spleen and liver  and  sometimes  early death.  An estimated
15,000 people suffer from Gaucher disease in the United  States,  of whom 2,000
to  3,000 require medical attention.  Genetically-engineered glucocerebrosidase
is designed  to  replace  the  missing  enzyme.   Enzon  and  scientists at the
National Institute of Mental Health, a division of the NIH, have  been  working
on   a  PEG-modified  version  of  glucocerebrosidase  under  a  November  1991
Cooperative  Research  and  Development  Agreement ("CRADA").  During September
1994,  the  Company  began  a  Phase  I clinical  trial  in  Gaucher  patients.
Currently, two patients are enrolled in  this trial and additional patients are
anticipated to be added when clinical trial material becomes available.

ONCOLOGY

      The  Company  has  several products under  development  in  the  area  of
oncology, all of which are in the early research stage.  These products include
PEG modified anti-cancer compounds and a novel chemical compound.

STRATEGIC ALLIANCES AND LICENSE AGREEMENTS

      Enzon develops and manufactures,  under  joint  arrangements  with  other
pharmaceutical   and   biopharmaceutical   companies,   protein-based  products
utilizing its proprietary PEG and SCA technologies.  Enzon  believes  that  its
technologies can be used to improve products which are already on the market or
that  are  under  development,  thus  producing therapeutic products which will
provide a safer, more effective and more convenient therapy.

      Enzon's agreements with its strategic  alliance partners provide, in most
cases, for Enzon's partners to pay the costs of  development, clinical testing,
obtaining  regulatory  approval and commercialization  of  the  products.   The
alliance partner receives  marketing  rights,  and  in some cases manufacturing
rights,  to  the  products  developed.   Enzon  receives  milestone   payments,
manufacturing  revenues  and/or  royalty payments based on product sales.   The
following is a list of certain of the Company's strategic alliance partners:

CORPORATE PARTNER AGREEMENT DATE PRODUCT DISEASE OR INDICATIONPROGRAM STATUS
Sanofi Winthrop, Inc. June 1989 PEG-SOD Closed Head Phase III (formerly Sterling Winthrop, Inc.) Injury Clinical Trials Schering Corporation November 1990/ PEG-INTRON A Various Phase I June 1995 Clinical Trials Baxter Healthcare CorporationNovember 1992 SCA proteins Cancer Research Eli Lilly and Co. December 1992 SCA proteins Undetermined Research Bristol-Myers Squibb, Inc. September 1993/ SCA proteins All TherapeuticsResearch July 1994
SANOFI AGREEMENT In June 1989, Enzon granted to Sanofi (the "Sanofi Agreement") the exclusive worldwide marketing rights, foreign regulatory approval responsibility and foreign manufacturing rights for PEG-SOD, which is the enzyme SOD modified by the PEG Process. SOD destroys oxygen free radicals that may damage tissue during reperfusion associated with myocardial infarction, organ transplant and trauma. Generally, Enzon will be entitled to 40% of the net profits from sales of PEG-SOD in the United States during the life of the basic U.S. PEG patent covering the product, with agreed-upon limits on the amount of expenses that can be deducted by Sanofi from revenues before calculating the profit split. Sanofi is presently developing PEG-SOD, which it has trademarked as DISMUTEC, for closed head trauma. Sanofi has advised the Company that it is currently conducting an expanded Phase III clinical trial on PEG-SOD, which is expected to be completed during the fourth quarter of 1995. A smaller, double blind, Phase III study with approximately 460 patients has been completed. This study showed that patients receiving DISMUTEC showed 18% and 16% relative improvement in favorable neurological outcomes compared to patients receiving a placebo three and six months after injury, respectively. Published sources indicate that the FDA has granted PEG-SOD "fast track" status in the FDA's new drug approval process. Under the Sanofi Agreement, Enzon is entitled to manufacture PEG-SOD for United States sales by Sanofi; however, Sanofi has the right to take over such manufacturing or have such manufacturing performed on its behalf in consideration for the payment, under certain circumstances, of an additional royalty. Sanofi is manufacturing the PEG-SOD utilized in its clinical trials and the Company expects that Sanofi will manufacture the product for U.S. sales if it is approved by the FDA. All development and regulatory approval costs for PEG-SOD, including the cost of unmodified enzymes for the product used in pre-approval testing are to be borne by Sanofi. The Sanofi Agreement terminates on a country by country basis upon the expiration of the last to expire of the patents licensed to the Company under its license agreement with RCT. The United States patent licensed to Enzon under its agreement with RCT expires in December 1996. The Company has entered into an agreement with RCT to seek an extension of this patent for up to five years. The foreign patents covered by this license expired in earlier years, see "Patents". Upon such patent expiration or termination of the Sanofi Agreement due to the Company's breach of the agreement or bankruptcy, the license granted to Sanofi automatically converts to a non-exclusive, royalty- free, paid-up license, except that Sanofi may maintain an exclusive license with respect to PEG-SOD by paying the Company a reduced royalty on Sanofi's sales of PEG-SOD. Sanofi has the right to terminate the Sanofi Agreement at any time with respect to any or all of the countries which are covered by the agreement with no further obligation to the Company, in which case all rights terminated by Sanofi in this manner shall revert to the Company. For information regarding certain agreements between Enzon and RCT with respect to the extension of the patent which is the subject of Enzon's license agreement with Sanofi, see "Patents". SCHERING AGREEMENT In November 1990, Enzon and Schering Corporation ("Schering"), a subsidiary of Schering-Plough Corporation, signed an agreement (the "Schering Agreement") to apply the PEG Process to Schering's INTRON A (interferon alfa 2b), a genetically-engineered anticancer and antiviral drug. According to published sources, INTRON A, as it is currently formulated, must be administered at least three times a week by injection and can produce side effects such as fever and occasionally depressed blood count. A PEG form of INTRON A would be designed to improve the administration regimen by increasing the product's blood circulating life. INTRON A is currently approved in the United States for use in chronic hepatitis B, chronic hepatitis C, AIDS-related Kaposi's sarcoma, venereal warts and hairy cell leukemia. It is approved for use in 65 countries for a total of 16 disease indications. Schering-Plough Corporation reported 1994 INTRON A sales of $426,000,000 worldwide. In August 1992, a Phase I human clinical trial began using PEG-INTRON A for the indication of hepatitis. The protocol for that trial was completed. Schering and Enzon amended the Schering Agreement to develop a PEG-INTRON A formulation having improved performance characteristics. Pursuant to the amended agreement, the Company has prepared and delivered several PEG-INTRON A formulations for Schering's evaluation for additional clinical trials. On June 30, 1995, the Company and Schering further amended the Schering Agreement pursuant to which Enzon agreed to transfer proprietary know-how and manufacturing rights for PEG-INTRON A to Schering for $3,000,000, of which $2,000,000 was paid on June 30, 1995 and $1,000,000 will be paid upon completion of the know-how transfer, as defined in such amended agreements. In connection with the amendment, the Company also sold to Schering approximately 847,000 shares of unregistered, newly issued Common Stock for $2,000,000 in gross proceeds. Under the current Schering Agreement, Enzon retained an option to become Schering's exclusive manufacturer of PEG-INTRON A for the United States market upon FDA approval of such product. Under the Schering Agreement, Enzon is entitled to receive sequential payments, totalling approximately $6,000,000, subject to the achievement of certain milestones in the product's development program, as well as payments for the clinical material it produces. During the year ended June 30, 1992, the Company received the first milestone payment of $450,000 related to the filing of an Investigational New Drug Application. The Company will also receive royalties on worldwide sales of PEG-INTRON A, if any. Schering will be responsible for conducting and funding the clinical studies, obtaining regulatory approval and marketing the product worldwide on an exclusive basis. The Schering Agreement terminates, on a country-by-country basis, upon the expiration of the last to expire of any future patents covering the product which may be issued to Enzon, or 15 years after the product is approved for commercial sale, whichever shall be the later to occur. This agreement is subject to Schering's right of early termination if the product does not meet specifications, or if Enzon fails to obtain or maintain the requisite product liability insurance, or if Schering makes certain payments to Enzon. If Schering terminates the agreement because the product does not meet specifications, Enzon may be required to refund certain of the milestone payments. BRISTOL-MYERS AGREEMENT In September 1993, the Company and Bristol-Myers signed a license agreement for Enzon's SCA protein technology granting Bristol-Myers a world- wide, semi-exclusive license for a particular antigen. Bristol-Myers will apply the technology to develop cancer therapies based on antibodies targeting certain cancer cells. Under the agreement, Enzon is entitled to receive certain upfront payments and sequential payments, subject to the achievement of certain milestones in the development program. Bristol-Myers will have the right to manufacture and market products which it develops and Enzon will receive certain royalties on Bristol-Myers sales, if any. In July 1994, Bristol-Myers paid $1,800,000 to Enzon and exercised an option under the contract to acquire a world-wide non-exclusive license for SCA protein technology. The non-exclusive license is for all therapeutic fields. BAXTER AGREEMENT In November 1992, Enzon and Baxter signed an agreement granting Baxter a non-exclusive worldwide license to Enzon's SCA protein technology. It is anticipated that Baxter will use the SCA proteins in its cancer research programs focusing on human stem cell isolation and gene therapy. Under the agreement, Enzon is entitled to receive certain upfront payments and sequential payments, subject to the achievement of certain milestones in the development programs. Baxter will have the exclusive worldwide right to manufacture and market any products which it develops and Enzon will receive certain royalties on Baxter's sales, if any. ELI LILLY (HYBRITECH) AGREEMENT In December 1992, Enzon and Hybritech Incorporated ("Hybritech"), a subsidiary of Eli Lilly, signed an agreement granting Hybritech a non-exclusive worldwide license to Enzon's SCA protein technology. Hybritech subsequently assigned this agreement to Eli Lilly. Under the agreement, Enzon is entitled to certain upfront payments totaling $1,200,000, of which $700,000 and $500,000 were received during the fiscal years ended June 30, 1994 and 1993, respectively, and is entitled to receive certain royalties on sales of products that may be developed using Enzon's SCA protein technology. MARKETING Other than ADAGEN, which the Company markets on a worldwide basis to a small patient population, the Company does not engage in the direct commercial marketing of any of its products and therefore does not have an established sales force. For certain of its products, the Company has provided exclusive marketing rights to its corporate partners in return for royalties to be received on sales. With respect to ONCASPAR, the Company has granted RPR exclusive marketing rights in North America pursuant to the agreements described in "Products on the Market - ONCASPAR". The Company expects to retain marketing partners to market ONCASPAR in other foreign markets and is currently pursuing arrangements in this regard. There can be no assurance that the Company will conclude any such arrangements. Regarding the marketing of certain of the Company's other future products, the Company expects to evaluate whether to create a sales force to market certain products in the United States or to continue to enter into license and marketing agreements with others for United States and foreign markets. These agreements generally provide that all or a significant portion of the marketing of these products will be conducted by the Company's licensees or marketing partners. In addition, under certain of these agreements, the Company's licensee or marketing partner may have all or a significant portion of the development and regulatory approval responsibilities. RAW MATERIALS AND MANUFACTURING In the manufacture of its products, the Company couples activated forms of PEG to the unmodified proteins. In the case of PEG, the Company does not have a long-term supply agreement, but maintains what it believes to be an adequate inventory which should provide the Company sufficient time to find an alternate supply of PEG, in the event it becomes necessary, without material disruption of its business. With respect to Enzon's manufacturing facilities, prior to the approval of both ADAGEN and ONCASPAR, the Company's manufacturing facility was inspected by the FDA for compliance with its guidelines for current good manufacturing practices. Although the Company is currently producing many of the unmodified proteins utilized in products it has under development, including purified bovine hemoglobin for use in its PEG-hemoglobin product, it may be required to obtain supply contracts with outside suppliers for certain unmodified proteins. The Company does not produce the unmodified adenosine deaminase used in the manufacture of ADAGEN and the unmodified L-asparaginase used in the manufacture of ONCASPAR and has a supply contract with an outside supplier for each of these unmodified proteins. The supply contract for unmodified L- asparaginase contains minimum purchase requirements. Under the Sanofi Agreement, in the event Sanofi decides to have the Company manufacture PEG-SOD, which the Company believes is unlikely, it will be the responsibility of Sanofi to provide the Company with unmodified SOD as needed. Schering is required under the Schering Agreement to provide the Company with unmodified INTRON A if the Company exercises its option to manufacturer PEG-INTRON A for the United States market. The Company currently manufactures the unmodified protein used in PEG- glucocerebrosidase, which is currently in clinical trials. There can be no assurance that the unmodified protein used in the manufacture of PEG- glucocerebrosidase can be produced in the amounts necessary to expand the current clinical trials. Delays in obtaining or an inability to obtain any unmodified protein which the Company does not produce, including unmodified adenosine deaminase or L-asparaginase, could have a material adverse effect on the Company. In the event the Company is required to locate an alternate supplier for an unmodified protein utilized in a product which is being sold commercially or which is in clinical development, the Company will likely be required to do additional testing, which could cause delay and additional expense, to demonstrate that the alternate supplier's material is biologically and chemically equivalent to the unmodified protein previously used. Such evaluations could include one or all of the following: chemical, pre-clinical and clinical studies. Requirements for such evaluations would be determined by the stage of the product's development and the reviewing division of the FDA. If such alternate material is not demonstrated to be chemically and biologically equivalent to the previously used unmodified protein, the Company will likely be required to repeat some or all of the pre-clinical and clinical trials with such protein. The marketing of an FDA approved drug could be disrupted while such tests are conducted. Even if the alternate material is shown to be chemically and biologically equivalent to the previously used protein, the FDA may require the Company to conduct additional clinical trials with such alternate material. GOVERNMENT REGULATION The manufacturing and marketing of pharmaceutical products in the United States requires the approval of the FDA under the Federal Food, Drug and Cosmetic Act. Similar approvals by comparable agencies are required in most foreign countries. The FDA has established mandatory procedures and safety standards which apply to the clinical testing, manufacture and marketing of pharmaceutical products. Obtaining FDA approval for a new therapeutic may take several years and involve substantial expenditures. Pharmaceutical manufacturing facilities are also regulated by state, local and other authorities. As an initial step in the FDA regulatory approval process, pre-clinical studies are conducted in animal models to assess the drug's efficacy and to identify potential safety problems. The results of these studies are submitted to the FDA as a part of the Investigational New Drug Application ("IND"), which is filed to obtain approval to begin human clinical testing. The human clinical testing program may involve up to three phases. Data from human trials are submitted to the FDA in a New Drug Application ("NDA") or Product License Application ("PLA"). Preparing an NDA or PLA involves considerable data collection, verification and analysis. ONCASPAR and ADAGEN received FDA marketing approval in February 1994 and March 1990, respectively. None of the Company's other products has received FDA marketing approval. Difficulties or unanticipated costs may be encountered by the Company or its licensees or marketing partners in their respective efforts to secure necessary governmental approvals, which could delay or preclude the Company or its licensees or marketing partners from marketing their products. With respect to patented products, delays imposed by the government approval process may materially reduce the period during which the Company will have the exclusive right to exploit them. See "Patents". COMPETITION Many established biotechnology and pharmaceutical companies with greater resources than the Company are engaged in activities that are competitive with those of Enzon and may develop products or technologies which compete with those of the Company. Although Enzon believes that the experience of its personnel in biotechnology, the patent under which the Company has a license from Research Corporation, other patents which have been licensed by or issued to the Company and the proprietary know-how developed by the Company provide it with a competitive advantage in its field, there can be no assurance that the Company will be able to maintain any competitive advantage, should it exist, in view of the greater size and resources of many of the Company's competitors. Research Corporation has in the past, and may in the future, license to other parties products under the original patent which are not already licensed or reserved for license to the Company. Enzon is aware that other companies are conducting research on chemically modified therapeutic proteins and that certain companies are modifying pharmaceutical products, including proteins, by attaching PEG. While the Company believes that products modified with its PEG Process are superior to these other products, there is no assurance that this will prove to be the case. Other than the Company's products ONCASPAR and ADAGEN, the Company is unaware of any PEG-modified therapeutic proteins which are currently available commercially for therapeutic use. Nevertheless, other drugs or treatment modalities which are currently available or that may be developed in the future, and which treat the same diseases as those which the Company's products are designed to treat, may be competitive with the Company's products. Prior to the development of ADAGEN, the Company's first FDA approved product, the only treatment available to patients afflicted with SCID was bone marrow transplants. Completing a successful transplant depends upon finding a matched donor, the probability of which is low. More recently, researchers at the NIH have been attempting to treat SCID patients with gene therapy, which if successfully developed, would compete with, and could eventually replace ADAGEN as a treatment. The theory behind gene therapy is that cultured T-lymphocytes injected back into the patient will express permanently and at normal levels, adenosine deaminase, the deficient enzyme in people afflicted with SCID. To date, gene therapy clinical trials have not been conclusive. Those patients currently being treated with gene therapy have continued to be treated with ADAGEN. Current standard treatment of patients with ALL includes administering unmodified L-asparaginase along with the drugs vincristine, prednisone and daunomycin. Recent studies have shown that long-term treatment with L-asparaginase increases the disease free survival in high risk patients. ONCASPAR, the Company's PEG-modified L-asparaginase product, is used to treat patients with ALL who are hypersensitive (allergic) to unmodified forms of L-asparaginase. The long-term survival and cure of ALL patients depends upon achieving a sustainable first remission. Currently, there are two unmodified forms of L-asparaginase available in the United States -- Elspar and Erwinase. The Company believes that ONCASPAR has the following two advantages over these unmodified forms of L-asparaginase: increased circulating blood life and generally reduced immunogenicity. Several companies are actively pursuing the development of a blood substitute and certain of these products are currently also being tested in clinical trials. Companies developing a hemoglobin-based product have researched the use of human, bovine, genetically engineered and transgenic hemoglobin. Each source of hemoglobin has various problems associated with it. The use of outdated human donor blood relies on a hemoglobin source which is at risk, both in terms of safety and supply availability. In the case of non-human or mutant (genetically engineered) hemoglobin, there is a risk of eliciting an immunogenic or allergic response to what the body considers to be a foreign protein. The Company believes that the use of genetic engineering techniques to produce a safe hemoglobin in commercial quantities will require the development of manufacturing capabilities which to date have generally not been demonstrated. Enzon believes its PEG-hemoglobin product will address the problems of immunogenicity and transfer of human disease, and further enable the Company to manufacture large quantities of the product. The Company is also aware of competitors who have conducted clinical trials on bovine-based hemoglobin-based oxygen carriers. There can be no assurance that such competing products will not be approved for sale by the FDA before the Company's product. Certain of the Company's competitors are attempting to develop oxygen carriers using perfluorocarbons ("PFC"). The FDA has allowed PFC trials only for very limited applications where benefits may be realized from localized, short-term use of very small amounts of the substance. PFCs are currently approved by the FDA for limited use in angioplasty patients. Clinical trials of PFC-based oxygen carriers for treatment of anemia were halted prior to completion. PEG-glucocerebrosidase is being developed by the Company and is intended to treat Gaucher disease. The FDA has granted Orphan Drug designation for the Company's PEG-glucocerebrosidase. In the event PEG-glucocerebrosidase is developed successfully, it would compete with CEREDASE, an FDA approved product, which is derived from human placental tissue, marketed by Genzyme Corporation ("Genzyme"), for the treatment of Gaucher disease. Genzyme received FDA approval for CEREDASE in April 1991. Genzyme also has received FDA marketing approval for a recombinant glucocerebrosidase. PEG-glucocerebrosidase would be designed to reduce the frequency of dosage and improve the method of administration by increasing the product's blood circulating life. There are several technologies which compete with the Company's SCA technology, including chimeric antibodies, humanized antibodies, human monoclonal antibodies, recombinant antibody FAB fragments, low molecular weight peptides and mimetics. These competing technologies can be categorized into two areas: (i) those modifying the monoclonal to minimize immunological reaction to a foreign protein, which is the strategy employed with chimerics, humanized antibodies and human monoclonal antibodies, and (ii) those creating smaller portions of the monoclonal which are more specific to the target and have fewer side effects, as is the case with FAB fragments and low molecular weight peptides. Enzon believes that the smaller size of its SCA proteins should permit better penetration into the tumor, result in rapid clearance from the blood and cause a significant decrease in the immunogenic problems associated with conventional monoclonal antibodies. A number of companies have active programs in SCA proteins. The Company believes that its patent position on SCA proteins will require these other companies to obtain licenses from Enzon, in order to commercialize their products, but there can be no assurance that this will prove to be the case. RESEARCH CORPORATION LICENSE AGREEMENTS On December 18, 1979, the United States Patent and Trademark Office issued a patent encompassing the PEG Process (Non-Immunogenic Polypeptides, Patent No. 4,179,337) to one of the Company's co-founders, Frank F. Davis, Ph.D., and two other inventors who are unaffiliated with the Company. Dr. Davis and his co-inventors were all professors at Rutgers University in New Brunswick, New Jersey at the time the patent was issued. The patent was transferred from Rutgers University to RCT, a not-for-profit corporation, pursuant to an agreement between Rutgers University and RCT requiring such transfer in return for RCT's paying the costs associated with obtaining the patent and making certain royalty payments to the inventors. RCT then granted certain licenses under the patent to Enzon, which was formed by Dr. Abraham Abuchowski and Dr. Davis to commercialize the PEG Process. Under the license agreement between the Company and RCT, dated August 25, 1985, and as amended on May 3, 1989, RCT granted the Company an exclusive license, with the right to sublicense, to make, use and sell certain products utilizing the PEG Process as set forth in the original patent held by RCT in countries in which a patent exists or a patent application has been filed by RCT. Under this license agreement, the Company has obtained such a license for seven specific products, has the right to use limited research quantities of non-licensed enzymes, and has the option to include all other enzymes, except allergens and lymphokines, under this license by paying RCT an option fee. The Company has certain diligence obligations to obtain regulatory approval of the licensed products in those countries in which patents covering the PEG Process have been issued, including obtaining FDA approval in the United States, and to sell the licensed products once such approvals are obtained. Enzon entered into another license agreement with RCT in September 1989, under which Enzon was granted an exclusive license under the patent covered by the License Agreement, with the right to sublicense, to make, use, and sell products in eight additional fields. The Company also has the option to license several other products. The Company has exercised this option for PEG- glucocerebrosidase and PEG-alpha-galactosidase. The terms of this license agreement are similar to the terms of the original license agreement, except that the Company has expanded rights to enforce the licensed patents for these products. See "Patents". The Company and RCT have signed agreements seeking to extend the PEG patent for PEG-SOD. Under United States patent laws, interim patent extension is available for PEG-SOD, provided a NDA is filed before scheduled expiration of the patent at the end of 1996, and other requirements of the law are met. A final extension is available upon FDA approval of the product. Under the agreements with RCT, Enzon will also pay RCT a royalty on sales of ONCASPAR until 1999. RCT has in the past, and may in the future, license products to other parties under the original patent covered by its license agreement with the Company which are not already licensed or reserved to the Company. PATENTS The Company has licensed, and been issued, a number of patents in the United States and other countries and has other patent applications pending to protect its proprietary technology. Although the Company believes that its patents provide adequate protection for the conduct of its business there can be no assurance that such patents will be of substantial protection or commercial benefit to the Company, will afford the Company adequate protection from competing products, will not be challenged or declared invalid, or that additional United States patents or foreign patent equivalents will be issued to the Company. The degree of patent protection to be afforded to biotechnological inventions is uncertain and the Company's products are subject to this uncertainty. The Company is aware of certain issued patents and patent applications, and there may be other patents and applications, containing subject matter which the Company or its licensees or collaborators may require in order to research, develop or commercialize at least some of the Company's products. There can be no assurance that licenses under such subject matter will be available on acceptable terms. One such patent is U.S. Patent No. 5,084,558, which issued on January 28, 1992, and is entitled "Extra Pure Semi-Synthetic Blood Substitute". It could be asserted that this patent includes claims which would cover the Company's PEG-hemoglobin product. In the opinion of the Company and the Company's outside patent counsel, Lerner, David, Littenberg, Krumholz and Mentlik, the Company's PEG-hemoglobin product does not infringe any claim of such patent which would be held valid if litigated. However, there can be no assurance that a court would find any of the claims of such patent to be invalid, that a court would not hold that the Company's PEG-hemoglobin product does infringe one or more valid claims of such patent, or that a license could be obtained under such patent on acceptable terms. The Company expects that there may be significant litigation in the industry regarding patents and other proprietary rights and, if Enzon were to become involved in such litigation, it could consume a substantial amount of the Company's resources. In addition, the Company relies heavily on its proprietary technologies for which pending patent applications have been filed and on unpatented know-how developed by the Company. Insofar as the Company relies on trade secrets and unpatented know-how to maintain its competitive technological position, there can be no assurance that others may not independently develop the same or similar technologies. Although the Company has taken steps to protect its trade secrets and unpatented know-how, third-parties nonetheless may gain access to such information. RCT holds the original patents upon which the PEG Process is based. The Company's ability to market certain of its PEG products is dependent upon its license agreements with RCT under these patents. Although the Company has licensed certain products covered by the patents held by RCT, there can be no assurance that these patents will enable the Company or RCT to prevent infringement or that competitors will not develop competitive products outside the protection that may be afforded by these patents. RCT's patent in the United States expires in December 1996 and its patents in certain foreign countries have expired or will expire in the remainder of 1995. The Company is aware that others have also filed patent applications and have been granted patents in the United States and other countries with respect to the application of PEG to proteins. The Company is permitted, under certain circumstances, to enforce the patents for certain of the products covered by the license agreements with RCT. Generally, however, under the terms of its license agreements with RCT, the Company cannot commence any action to prosecute any infringement of the patents and must rely upon RCT to do so. If RCT is unwilling or unable to bring such a suit, the Company may be precluded from doing so and its business may be materially adversely affected. Even if the Company were permitted under its agreements with RCT to prosecute a patent infringement action, it may not have the resources to do so. In the field of SCA proteins, the Company has several United States and foreign patents and patent applications, including a patent granted in August 1990 covering the genes needed to encode SCA proteins. Creative BioMolecules, Inc. ("Creative") provoked an interference with the patent and on June 28, 1991, the United States Patent and Trademark Office entered summary judgment terminating the interference proceeding and upholding the Company's patent. Creative subsequently lost its appeal of this decision in the United States Court of Appeals. Creative did not file a petition for review of this decision by the United States Supreme Court within the required time period. In November 1993, Enzon and Creative signed collaborative agreements in the field of Enzon's SCA protein technology and Creative's Biosynthetic Antibody Binding Site (BABS) protein technology. Under the agreements, each company is free, under a non-exclusive, worldwide license, to develop and sell products utilizing the technology claimed by both companies' antigen binding engineering patents, without paying royalties to the other. Each is also free to market products in collaboration with third parties, but the third parties will be required to pay royalties on products covered by the patents which will be shared by the companies, except in certain instances. Enzon has the exclusive right to market licenses under both companies' patents other than to Creative's collaborators. In addition, the agreements provide for the release and discharge by each company of the other, from any and all claims based on past infringement of the technology which is the subject of the agreements. The agreement also provides for any future disputes between the companies, regarding new patents in the area of engineered monoclonal antibodies, to be resolved pursuant to agreed upon procedures. Although the Company believes that its patents provide adequate protection for the conduct of its business as described herein, there can be no assurance that such patents will be of substantial protection from competing products, will not be challenged or declared invalid, or that additional United States patents or foreign patent equivalents will be issued to the Company. EMPLOYEES As of June 30, 1995, Enzon employed 123 persons, of whom 61 were engaged in research and development activities, 36 were engaged in manufacturing, and 26 were engaged in administration and management. As of June 30, 1995, the Company had 25 employees who hold Ph.D. degrees. The Company believes that it has been highly successful in attracting skilled and experienced scientific personnel; however, competition for such personnel is intensifying. None of the Company's employees are covered by a collective bargaining agreement. All of the Company's employees are covered by confidentiality agreements. Enzon considers relations with its employees to be good. ITEM 2. PROPERTIES The Company owns no real property. The following are all of the facilities that Enzon currently leases: APPROX. APPROX. PRINCIPAL SQUARE ANNUAL LEASE LOCATION OPERATIONS FOOTAGE RENT EXPIRATION 20 Kingsbridge RoadResearch & Development56,000$440,000(1) June 16, 2007 Piscataway, NJ and Administrative
40 Cragwood Road Research & 88,000 792,000(2) December 31, 1998
S. Plainfield, NJDevelopment, Pilot Scale Manufacturing
300 Corporate Ct.Manufacturing 24,000 135,000(3) November 30, 1998
S. Plainfield, NJ (1) Under the terms of the lease, annual rent increases over the term of the lease from $440,000 to $581,000. (2) Net of subrental income of $242,000; the sublease is for approximately 24,312 square feet. (3) Net of subrental income of $48,000; the sublease is for approximately 6,000 square feet. The Company believes that its facilities are well maintained and generally adequate for its present and future anticipated needs. During fiscal 1995, the Company terminated its lease for its 40 Kingsbridge Road facility which was scheduled to expire in 2007, in return for the surrender of the $600,000 security deposit on the building. ITEM 3. LEGAL PROCEEDINGS There is no material litigation pending to which the Company is a party or to which any of its property is subject. ITEM 4. SUBMISSION OF MATTERS TO A VOTE OF SECURITY HOLDERS None. PART II ITEM 5. MARKET FOR THE REGISTRANT'S COMMON EQUITY AND RELATED STOCKHOLDER MATTERS The Company's Common Stock is traded in the over-the-counter market and is quoted on the NASDAQ National Market System under the trading symbol "ENZN". The following table sets forth the high and low sale prices for the Common Stock for the years ended June 30, 1995 and 1994, as reported by the NASDAQ National Market System. The quotations shown represent inter-dealer prices without adjustment for retail mark-ups, mark downs or commissions, and may not necessarily reflect actual transactions. HIGH LOW Year Ended June 30, 1995 First Quarter 3 1/4 2 1/8 Second Quarter 3 1/8 1 1/2 Third Quarter 2 1/2 1 11/16 Fourth Quarter 2 7/8 1 3/4 Year Ended June 30, 1994 First Quarter 6 3/8 4 1/8 Second Quarter 6 1/4 4 3/8 Third Quarter 5 5/8 4 1/8 Fourth Quarter 4 3/8 2 As of September 15, 1995 there were 3,235 holders of record of the Common Stock. The Company has paid no dividends on its Common Stock since its inception and does not plan to pay dividends on its Common Stock in the foreseeable future. Except as may be utilized to pay dividends payable on the Company's outstanding Series A Cumulative Convertible Preferred Stock ("Series A Preferred Shares" or "Series A Preferred Stock"), any earnings which the Company may realize will be retained to finance the growth of the Company. In addition, no dividends may be paid or set apart for payment on the Common Stock unless the Company shall have paid in full, or made appropriate provision for the payment in full of, all dividends which have then accumulated on the Series A Preferred Shares. ITEM 6. SELECTED FINANCIAL DATA Set forth below is the selected financial data for the Company for the five fiscal years ended June 30, 1995. CONSOLIDATED STATEMENT OF OPERATIONS DATA: YEAR ENDED JUNE 30,
1991 1992 1993 1994 1995 Revenues $ 2,410,638$ 5,684,944$ 8,414,349 $ 14,797,499 $15,826,437 Net Loss $(11,960,760)$(28,182,829) $(24,601,310) $(16,495,226) $(6,291,491) Net Loss per Share$ ( .90)$ (1.46)$ (1.15)$ (.71)$ (.26)
Dividends on
Common Stock None None None None None
CONSOLIDATED BALANCE SHEET DATA: JUNE 30,
1991 1992 1993 1994 1995 Total Assets $ 54,205,130 $39,310,862 $33,920,859 $20,543,252 $19,184,042
Long-Term
Obligations None $ 232,958 $ 141,772 $ 115,733 $ 4,076
ITEM 7. MANAGEMENT'S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS RESULTS OF OPERATIONS FISCAL YEARS ENDED JUNE 30, 1995, 1994 AND 1993 REVENUES. The components of revenues for the last three fiscal years have principally been sales and contract revenues. Revenues for the fiscal year ended June 30, 1995 increased by 7% to $15,826,000 as compared to $14,797,000 for fiscal 1994. Sales increased by 35% to $11,024,000 for the year ended June 30, 1995 as compared to $8,182,000 for the prior year, due to the shipment of clinical material to Schering, an increase in patients receiving ADAGEN and increased ONCASPAR revenues from RPR. The Company has no firm orders for additional clinical supplies from Schering. ADAGEN sales for the years ended June 30, 1995 and 1994 were $8,305,000 and $7,601,000, respectively. Contract revenue for the year ended June 30, 1995 decreased by 27% to $4,802,000, as compared to $6,616,000 for fiscal 1994. The decrease was principally due to a one time payment received during fiscal 1994 from RPR related to the FDA approval of ONCASPAR. The decrease was offset in part by a payment of $1,800,000 recorded in fiscal 1995 from Bristol-Myers Squibb related to the exercise of its option under an agreement dated September 1993, to acquire a worldwide non-exclusive license for all therapeutic indications for the Company's SCA protein technology and $2,000,000 received related to the amendment of the Company's agreement with Schering. During the fiscal years ended June 30, 1995 and 1994, the Company had export sales of $2,105,000 and $2,085,000, respectively. Sales in Europe were $1,841,000 and $1,957,000 for the years ended June 30, 1995 and 1994, respectively. Revenues for fiscal 1994 increased by 76% to $14,797,000 as compared to $8,414,000 for fiscal 1993. Sales increased by 15% to $8,182,000 for fiscal 1994 as compared to $7,113,000 for the prior year, due primarily to an increase in patients receiving ADAGEN. The increase in sales of ADAGEN was offset in part by a reduction in shipments of clinical supplies to a collaborative partner, and a decrease in sales of the Company's software subsidiary, Symvex Inc., which was shut down during the year. ADAGEN sales for the fiscal years ended June 30, 1994 and 1993 were $7,601,000 and $5,788,000, respectively. During the fiscal years ended June 30, 1994 and 1993, the Company had export sales of $2,085,000 and $1,631,000, respectively. Sales in Europe were $1,957,000 and $1,346,000 for the fiscal years ended June 30, 1994 and 1993, respectively. Contract revenue for fiscal year 1994 increased by $5,405,000 to $6,616,000, primarily due to $5,500,000 in one time licensing fees received related to the FDA's approval of ONCASPAR under the Company's exclusive U.S. marketing rights license with RPR. COST OF SALES. Cost of sales, as a percentage of sales, for fiscal 1995 was 26% as compared to 27% in fiscal 1994. An increase in the charge to cost of goods sold related to idle capacity at the Company's manufacturing facility was offset by a decrease in the write-off of excess raw material (PEG). Prior to the approval of ONCASPAR, the Company's first FDA approved drug for a potentially large patient population, idle capacity was charged to research and development expense. During the fiscal year ended June 30, 1995, the Company utilized approximately 36% of its manufacturing capacity for its approved products, ADAGEN and ONCASPAR, as well as clinical material for its collaborative partner, Schering Corporation. Cost of sales, as a percentage of sales, increased to 27% in fiscal 1994 as compared to 15% in fiscal 1993. The increase was due to (i) the write-off of excess raw material (PEG), which would expire in the next year, and (ii) a charge in the fourth quarter for idle capacity at the Company's manufacturing facility. In the fourth quarter of fiscal 1994, the Company began classifying idle capacity as cost of sales. Prior to the fourth quarter of 1994, idle capacity was charged to research and development expense. RESEARCH AND DEVELOPMENT. Research and development expenses in fiscal 1995 decreased by 32% to $12,084,000 as compared to $17,665,000 in fiscal 1994. The majority of the Company's research and development expenditures related to the continued development and clinical trials for PEG-hemoglobin and PEG- glucocerebrosidase. The decrease was principally due to (i) reductions in personnel, principally in the clinical and scientific administration areas, and related costs such as payroll taxes and benefits, (ii) decreased research facility and occupancy costs, (iii) the charging of idle capacity to cost of sales, rather than research and development, as was the case in the first nine months of fiscal 1994, and (iv) other cost containment measures implemented by the Company. The decreases in research facility and occupancy costs related to a one time credit received from one of the Company's landlords, the sublease of certain facilities and the termination of one of the Company's long-term facility leases and the resulting consolidation of its operations. Research and development expenses in fiscal 1994 remained relatively constant at $17,665,000 compared to $17,710,000 in fiscal 1993. Increased costs in the areas of (i) contracted services related to toxicology studies, (ii) wages and related benefits, and (iii) research facility and occupancy costs were offset by a reduction in the amount of idle manufacturing capacity during the first nine months of fiscal 1994 and other cost containment measures taken by the Company. Idle capacity was charged to research and development prior to the launch of ONCASPAR. SELLING, GENERAL AND ADMINISTRATIVE EXPENSES. Selling, general and administrative expenses for fiscal 1995 decreased by 41% to $6,916,000 from $11,710,000 for fiscal 1994. The decrease was due to (i) reductions in personnel and related costs, such as payroll taxes and benefits, (ii) decreased marketing and advertising costs for ONCASPAR as a result of the Company's license agreement with RPR, and (iii) other cost containment measures taken by the Company. Under the Company's exclusive U.S. marketing rights license, RPR is responsible for all marketing and advertising costs related to ONCASPAR. Selling, general and administrative expenses for fiscal 1994 decreased by 22% to $11,710,000 from $14,933,000 in fiscal 1993. The decrease was due to (i) reductions in personnel and related costs, such as payroll taxes and benefits, due to staff reductions, (ii) decreased marketing and advertising costs for ONCASPAR as a result of the RPR license agreement, (iii) a reduction in facility costs due to the closing of the Company's Gaithersburg, Maryland facility, and (iv) other cost containment measures taken by the Company. RESTRUCTURING EXPENSE. During the quarter ended March 31, 1995, the Company reduced its workforce by 22 employees. As a result of these reductions, the Company was able to terminate its lease for its administrative headquarters at 40 Kingsbridge Road, Piscataway, New Jersey. These operations were consolidated into the Company's research and development facility. As part of the termination agreement, the landlord was able to draw down on a $600,000 letter of credit that served as a security deposit on both of the buildings the Company occupied on Kingsbridge Road in Piscataway. This termination payment and severance related to the staff reduction as well as the write-off of leasehold improvements, moving expenses and commissions due the Company's real estate broker were recorded as restructuring expense during the year ended June 30, 1995. OTHER INCOME/EXPENSE. Other income/expense increased to $994,000 for fiscal 1995 as compared to $250,000 for fiscal 1994. The increase was principally due to an insurance settlement received during fiscal 1995 related to ADAGEN that was destroyed in shipment. Other income/expense decreased by 64% in fiscal 1994 as compared to the previous year, primarily due to a reduction in interest-bearing investments as well as a decrease in interest rates. LIQUIDITY AND CAPITAL RESOURCES Enzon had $8,103,000 in cash and cash equivalents as of June 30, 1995. The Company invests its excess cash in a portfolio of high-grade marketable securities and United States government-backed securities. The Company's cash reserves as of June 30, 1995 increased by $2,372,000 from June 30, 1994. The increase in cash reserves was attributable to the proceeds from the Company's public offering of its Common Stock, the sale/leaseback of certain research and development equipment, the private sale of Common Stock to Schering, and a royalty advance of $3,500,000 received related to the renegotiation of the Company's exclusive U.S. marketing rights license with RPR. These increases were offset in part by the funding of operations for fiscal 1995. During January 1995, the Company amended its exclusive U.S. marketing rights license with RPR for ONCASPAR. Under the amended agreement, Enzon will earn a royalty on net sales of ONCASPAR as opposed to 50% of net profits provided for under the original agreement. The amended agreement provides for a payment of $3,500,000 in advance royalties, which was received in January 1995. Royalties due under the amended agreement will be offset against a credit of $5,970,000, which represents the royalty advance plus reimbursement of certain amounts due RPR under the previous agreement and interest expense, before cash payments will be made for base royalties, as defined under the agreement. The royalty advance is shown as a long term liability, with the corresponding current portion included in accrued expenses, on the Consolidated Balance Sheet as of June 30, 1995 and will be reduced as royalties are recognized under the agreement. The Company's agreement with Sanofi requires a credit to Sanofi for monies not expended for the development of PEG-SOD under the Company's March 1987 stock purchase agreement with Eastman Kodak Company ("Kodak"), pursuant to which Kodak advanced the Company $9,000,000 to fund all activities to obtain FDA approval for this product and purchased 2,000,000 shares of the Company's Common Stock for $6,000,000. The Company believes that under the agreement, Sanofi may only apply the credit, shown as a current liability in the Consolidated Balance Sheet, against the purchase of clinical supplies and the Company has no other obligation to repay the credit to Sanofi. Sanofi has notified the Company that it does not require future clinical supplies from the Company and, therefore, the Company has no further obligation under the agreement to supply PEG-SOD to Sanofi. As of June 30, 1995, 940,808 shares of Series A Preferred Stock had been converted into 3,093,411 shares of Common Stock. Accrued dividends on the converted Series A Preferred Stock in the aggregate of $1,792,000 were settled by the issuance of 232,383 shares of Common Stock. The Company does not presently intend to pay cash dividends on the Series A Preferred Stock. As of June 30, 1995, there were $1,149,000 of accrued and unpaid dividends on the Series A Preferred Stock. Dividends accrue on the outstanding Series A Preferred Stock at the rate of $218,000 per year. To date, the Company's sources of cash have been the proceeds from the sale of its stock through public and private placements, sales of ADAGEN, sales of ONCASPAR, sales of its products for research purposes, contract research and development fees and technology transfer and license fees. The Company's current sources of liquidity are its cash, cash equivalents and interest earned on such cash reserves, sales of ADAGEN, sales of ONCASPAR, sales of its products for research purposes and license fees. Management believes that its current sources of liquidity will be sufficient to meet anticipated cash requirements through fiscal year end 1996. Upon exhaustion of the Company's current cash reserves, the Company's continued operations will depend on, among other things, its ability to realize significant revenues from the commercial sale of its products, raise additional funds through equity or debt financing, or obtain significant licensing, technology transfer or contract research and development fees. There can be no assurance that these sales, financings or revenue generating activities will be successful. In management's opinion, the effect of inflation on the Company's past operations has not been significant. ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA The response to this Item is submitted as a separate section of this report commencing on Page F-1. ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE Not applicable. PART III The information required by Item 10 - Directors and Executive Officers of the Registrant; Item 11 - Executive Compensation; Item 12 - Security Ownership of Certain Beneficial Owners and Management; and Item 13 - Certain Relationships and Related Transactions is incorporated into Part III of this Annual Report on Form 10-K by reference to the Company's Proxy Statement for the Annual Meeting of Stockholders scheduled to be held on December 5, 1995. PART IV ITEM 14. EXHIBITS, FINANCIAL STATEMENT SCHEDULES, AND REPORTS ON FORM 8-K (a)(1) and (2). The response to this portion of Item 14 is submitted as a separate section of this report commencing on page F-1. (a)(3) and (c). Exhibits (numbered in accordance with Item 601 of Regulation S-K).
Exhibit Page Number or NUMBER DESCRIPTION Incorporation BY REFERENCE 1.1 Form of Third Amended and Restated Purchase Agreement by and between the Company and Susquehanna Brokerage Services, Inc. dated as of June 24, 1994 ##(1.1) 4.0 Certificate of Designation for the Series A Cumulative Convertible Preferred Stock filed with the Secretary of State of Delaware *(4.0) 10.0 Employment Agreement dated March 25, 1994 with Peter G. Tombros #(10.17) 10.1 Termination Agreement and General Release dated May 17, 1994 with Edward Ehrenberg ###(10.3) 10.2 Form of Change of Control Agreements dated as of January 20, 1995 entered ~(10.2) into with the Company's Executive Officers 10.3 Lease - 300-C Corporate Court, South Plainfield, New Jersey ***(10.3) 10.4 Modification of Lease - 300-C Corporate Court, South Plainfield New Jersey ++(10.3) 10.5 Lease Termination Agreement dated March 31, 1995 for 20 Kingsbridge Road and 40 Kingsbridge Road, Piscataway, New Jersey ~(10.6) 10.6 Option Agreement dated April 1, 1995 regarding 20 Kingsbridge Road, Piscataway, New Jersey ~(10.7) 10.7 Lease - 20 Kingsbridge Road, Piscataway, New Jersey ~(10.8) 10.8 Form of Lease - 40 Cragwood Road, South Plainfield, New Jersey ****(10.9) 10.9 Lease 300A-B Corporate Court, South Plainfield, New Jersey (10.10) 10.10 Stock Purchase Agreement dated March 5, 1987 between the Company and Eastman Kodak Company ****(10.7) 10.11 Amendment dated June 19, 1989 to Stock Purchase Agreement between the Company and Eastman Kodak Company **(10.10) 10.12 Form of Stock Purchase Agreement between the Company and the purchasers of the Series A Cumulative Convertible Preferred Stock +(10.11) 10.13 Amendment to License Agreement and Revised License Agreement between the Company and RCT dated April 25, 1985 +++(10.5) 10.14 Amendment dated as of May 3, 1989 to Revised License Agreement dated April 25, 1985 between the Company and Research Corporation **(10.14) 10.15 License Agreement dated September 7, 1989 between the Company and Research Corporation Technologies, Inc. **(10.15) 10.16 Master Lease Agreement and Purchase Leaseback Agreement dated October 28, 1994 between the Company and Comdisco, Inc. ####(10.16) 10.17 Amendment dated as of May 15, 1995 to Employment Agreement with Peter G. Tombros E1 21.0 Subsidiaries of Registrant E2 23.0 Consent of KPMG Peat Marwick LLP E3 23.1 Consent of Lerner, David, Littenberg, Krumholz & Mentlik E4 27.0 Financial Data Schedule E5
* Previously filed as an exhibit to the Company's Registration Statement on Form S-2 (File No. 33-34874) and incorporated herein by reference thereto. ** Previously filed as exhibits to the Company's Annual Report on Form 10-K for the fiscal year ended June 30, 1989 and incorporated herein by reference thereto. *** Previously filed as an exhibit to the Company's Registration Statement on Form S-18 (File No. 2-88240-NY) and incorporated herein by reference thereto. **** Previously filed as exhibits to the Company's Registration Statement on Form S-1 (File No. 2-96279) filed with the Commission and incorporated herein by reference thereto. + Previously filed as an exhibit to the Company's Registration Statement on Form S-1 (File No. 33-39391) filed with the Commission and incorporated herein by reference thereto. ++ Previously filed as an exhibit to the Company's Annual Report on Form 10- K for the fiscal year ended June 30, 1992 and incorporated herein by reference thereto. +++ Previously filed as an exhibit to the Company's Annual Report on Form 10- K for the fiscal year ended June 30, 1985 and incorporated herein by reference thereto. # Previously filed as an exhibit to the Company's Current Report on Form 8- K dated April 5, 1994 and incorporated herein by reference thereto. ## Previously filed as an exhibit to the Company's Registration Statement on Form S-3 (File No. 33-80790) and incorporated herein by reference thereto. ### Previously filed as an exhibit to the Company's Annual Report on Form 10- K for the fiscal year ended June 30, 1994 and incorporated herein by reference thereto. #### Previously filed as an exhibit to the Company's quarterly report on Form 10-Q for the quarter ended December 31, 1994. ~ Previously filed as an exhibit to the Company's quarterly report on Form 10-Q for the quarter ended March 31, 1995. (b) Reports on Form 8-K On July 20, 1995, the Company filed with the Commission a Current Report on Form 8-K dated June 30, 1995, related to the Company and Schering executing an amendment to the license and development agreement between the Company and Schering, and the Company and Schering entering into a stock purchase agreement pursuant to which Schering purchased shares of the Company's Common Stock (Item 5). Signatures Pursuant to the requirements of Section 13 or 15(d) of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the undersigned, thereunto duly authorized. ENZON, INC. Dated: September 25, 1995 /S/ PETER G. TOMBROS By: Peter G. Tombros President and Chief Executive Officer Pursuant to the requirements of the Securities Exchange Act of 1934, this Annual Report has been signed below by the following persons on behalf of the Registrant and in the capacities and on the dates indicated: NAME TITLE DATE /S/ PETER G. TOMBROS President, Chief September 25, 1995 Peter G. Tombros Executive Officer and Director (Principal Executive Officer) /S/ KENNETH J. ZUERBLIS Vice President, Finance September 25, 1995 Kenneth J. Zuerblis (Principal Financial and Accounting Officer) /S/ ABRAHAM ABUCHOWSKI Chairman of the Board September 25, 1995 Abraham Abuchowski Director September 25, 1995 Rosina B. Dixon /S/ ROBERT LEBUHN Director September 25, 1995 Robert LeBuhn /S/ A.M. "DON" MACKINNON Director September 25, 1995 A.M. "Don" MacKinnon /S/ RANDY H. THURMAN Director September 25, 1995 Randy H. Thurman ENZON, INC. AND SUBSIDIARIES Index PAGE Independent Auditors' Report F-2 Consolidated Financial Statements: Consolidated Balance Sheets - June 30, 1995 and 1994 F-3 Consolidated Statements of Operations - Years ended June 30, 1995, 1994 and 1993 F-4 Consolidated Statements of Stockholders' Equity - Years ended June 30, 1995, 1994 and 1993 F-5 Consolidated Statements of Cash Flows - Years ended June 30, 1995, 1994 and 1993 F-7 Notes to Consolidated Financial Statements - Years ended June 30, 1995, 1994 and 1993 F-8 F-1 INDEPENDENT AUDITORS' REPORT The Board of Directors and Stockholders Enzon, Inc: We have audited the consolidated financial statements of Enzon, Inc. and subsidiaries as listed in the accompanying index. These consolidated financial statements are the responsibility of the Company's management. Our responsibility is to express an opinion on these consolidated financial statements based on our audits. We conducted our audits in accordance with generally accepted auditing standards. Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. An audit includes examining, on a test basis, evidence supporting the amounts and disclosures in the financial statements. An audit also includes assessing the accounting principles used and significant estimates made by management, as well as evaluating the overall financial statement presentation. We believe that our audits provide a reasonable basis for our opinion. In our opinion, the consolidated financial statements referred to above present fairly, in all material respects, the financial position of Enzon, Inc. and subsidiaries as of June 30, 1995 and 1994, and the results of their operations and their cash flows for each of the years in the three-year period ended June 30, 1995, in conformity with generally accepted accounting principles. /S/KPMG PEAT MARWICK LLP KPMG Peat Marwick LLP New York, New York September 21, 1995 F-2 ENZON, INC. AND SUBSIDIARIES CONSOLIDATED BALANCE SHEETS June 30, 1995 and 1994
ASSETS LIABILITIES AND STOCKHOLDERS' EQUITY 1995 1994 1995 1994 1994 Current assets: Current liabilities: Cash and cash $8,102,989 $5,731,461 Accounts payable $1,561,968$2,419,571 equivalents 2,362,277 1,928,453 Accrued expenses 4,045,3024,238,274 Accounts receivable 792,453 939,823 Other accrued liabilities - due to Sanofi 1,312,829 1,312,829 Inventories 9,6745,185 Accrued interest 175,552 107,330 Total current liabilities 6,920,099 7,970,674 receivable Prepaid expenses Total current assets 11,442,945 8,712,252 Accrued rent 1,006,508 1,860,782 Royalty advance - RPR 2,955,841 - Other liabilities 115,733 4,076 3,966,425 1,976,515 Property and equipment 15,758,058 17,606,217 Commitments and contingencies Less accumulated depreciation 9,968,024 8,386,254 Stockholders' equity: and amortization 5,790,034 9,219,963 Preferred stock-$.01 par value, authorized 3,000,000 shares; Other assets: issued and outstanding 109,000 shares in Investments 78,616 80,756 1995 and 1994 1,0901,090 Cash surrender value of (liquidation preference $25 per share life - 373,186 aggregating $2,725,000 insurance 46,627 170,935 in 1995 and 1994) 263,289244,273 Deposits and deferred 1,825,820 Common stock-$.01 par value, authorized 111,494,180107,520,250 charges 1,951,063 1,986,160 40,000,000 shares; (103,461,041) (97,169,550) Patents, net 2,611,037 issued and outstanding 26,328,874 shares in 1995 and 24,427,258 shares in 1994 Additional paid-in capital Accumulated deficit Total stockholders' equity 8,297,518 10,596,063 Total assets $19,184,042 $20,543,252 Total liabilities and stockholders' equity $19,184,042 $20,543,252
The accompanying notes are an integral part of these consolidated financial statements. F-3 ENZON, INC. AND SUBSIDIARIES CONSOLIDATED STATEMENTS OF OPERATIONS Years ended June 30, 1995, 1994 and 1993 YEARS ENDED JUNE 30,
1995 1994 1993 Revenues Sales $11,024,432 $8,181,999 $7,112,702 Grants - - 90,647 Contract revenue 4,802,005 6,615,500 1,211,000 Total revenues 15,826,437 14,797,499 8,414,349 Costs and expenses Cost of sales 2,918,737 2,168,3981,073,911 Research and development expenses 12,083,960 17,665,01417,709,805 Selling, general and administrative expenses 6,916,393 11,709,73514,932,960 Restructuring expense 1,192,971 - - Total costs and expenses 23,112,061 31,543,147 33,716,676 Operating loss (7,285,624) (16,745,648) (25,302,327) Other income (expense) Interest and dividend income 236,848 306,381749,340 Interest expense (3,988) (19,068) (48,323) Other 761,273 (36,891) - 994,133 250,422 701,017 Net loss ($6,291,491) ($16,495,226) ($24,601,310) Net loss per common share ($0.26) ($0.71) ($1.15) Weighted average number of common shares outstanding during the period 25,184,718 23,646,061 21,694,579
The accompanying notes are an integral part of these consolidated financial statements. F-4 ENZON, INC. AND SUBSIDIARIES CONSOLIDATED STATEMENTS OF STOCKHOLDERS' EQUITY Years ended June 30, 1995, 1994 and 1993
PREFERRED STOCK COMMON STOCK Additional Amount Number of Par Amount Number of Par paid-in Accumulated PER SHARE SHARES VALUE PER SHARE SHARES VALUE CAPITAL DEFICIT TOTAL Balance, July 1, 1992 Proceeds carried 131,000 109,000 $1,310 $1,090 Common stock issued for exercise from forward of public - - - $4.50 incentive stock options offering Common stock issued for exercise on - - - 4.12 of April non-qualified stock options 22, 1994 25.00 (14,000) (140) 8.27 Common stock issued on conversion Compensation - - - 8.27 of expense preferred stock related to - - - 6.05 Dividends issued on preferred vesting stock of stock - - - 8.88 Proceeds from public offering on options January 22, 1993 Common - - - 2.02 Common stock issued for stock - - - - acquisition issued for 117,0001,170 of Enzon Labs Inc. acquisition Issuance of common stock warrants of Enzon - - - 4.12 for Labs Inc. Enzon Labs Inc. Issuance 25.00 (8,000) (80) 9.10 Net loss of common - - - 9.10 Balance, June 30, 1993 stock Common stock issued for exercise warrants - - - 2.55 of for non-qualified stock options Enzon - - -- Common stock issued on conversion Labs Inc. of Net loss - - - 8.88 preferred stock Balance, Dividends issued on preferred June 30, - - - 2.02 stock 1994 - - - - 20,214,935 - $202,150 - $86,406,898 - ($55,925,014)($97,169,550)$30,685,344 3,00024,427,258 30 $244,273 13,470$107,520,250 - 13,500 25,300 253 104,072 - 104,325 42,320 423 (297) - (14) 10,157 101 83,896 (84,000) (3) 3,175,000 31,750 18,452,000 - 18,483,750 825 8 7,314 - 7,322 - - 1,390 - 1,390 - - - (24,601,310) (24,601,310) 23,471,537 234,715 105,068,743 (80,610,324) 24,694,304 140,850 1,409 578,942 - 580,351 21,978 220 (140) - - 7,032 70 63,921 (64,000) (9) 785,358 7,854 1,624,025 - 1,631,879 - - 179,465 - 179,465 503 5 4,459 - 4,464 - - 835 - 835 (16,495,226) (16,495,226) $10,596,063
The accompanying notes are an integral part of these consolidated financial statements. (continued) F-5 ENZON, INC. AND SUBSIDIARIES CONSOLIDATED STATEMENTS OF STOCKHOLDERS' EQUITY Years ended June 30, 1995, 1994 and 1993
PREFERRED STOCK COMMON STOCK Additional Amount Number of Par Amount Number of Par paid-in Accumulated PER SHARE SHARES VALUE PER SHARE SHARES VALUE CAPITAL DEFICIT TOTAL Balance, June 30, 1994 brought 109,000 $1,090 24,427,258 $244,273 $107,520,250($97,169,550)$10,596,063 forward Compensation expense related - - - - - - 31,535 -31,535 to vesting - - - 2.06 954,000 9,540 1,742,524 -1,752,064 of stock options Proceeds from public shelf - - - 2.25 100,000 1,000 224,000 -225,000 offering Common stock issued for - - - 2.36 847,489 8,475 1,974,575 -1,983,050 building purchase option - - - 8.88 127 1 1,126 -1,127 Common stock issued to Schering - - - 2.02 - - 170 -170 Corporation - - Common stock issued for - - - - - (6,291,491)(6,291,491) acquisition of 109,000 $263,289 Enzon Labs Inc. $1,090 26,328,874 $111,494,180($103,461,041)$8,297,518 Issuance of common stock warrants for Enzon Labs Inc. Net loss Balance, June 30, 1995
The accompanying notes are an integral part of these consolidated financial statements. F-6 ENZON, INC. AND SUBSIDIARIES CONSOLIDATED STATEMENTS OF CASH FLOWS Years Ended June 30, 1995, 1994 and 1993
YEARS ENDED JUNE 30, 1995 1994 1993 Cash flows from operating activities: Net loss ($6,291,491) ($16,495,226)($24,601,310) Adjustments to reconcile net loss to net cash used in operating activities: Depreciation and amortization 2,477,671 2,796,6542,557,250 Reserve for shutdown of Enzon Labs Inc. (71,743) (1,203,563)(24,694) Loss on retirement of equipment 9,003 38,8684,391 Compensation expense for issuance of stock options 31,535 179,465- Non-cash portion of restructuring expense 1,100,094 -- Changes in assets and liabilities: Increase in accounts receivable (433,824) (313,141)(939,467) Decrease in inventories 147,370 117,6149,515 (Increase) decrease in accrued interest receivable (4,489) 151,611294,045 (Increase) decrease in prepaid expenses (68,222) 222,179(14,790) Decrease (increase) in cash surrender value of life 67,871 (66,148) 10,356 insurance 126,448 5,303(81,560) Decrease (increase) in other assets (857,603) 407,433(362,170) (Decrease) increase in accounts payable (349,431) 1,200,481(77,511) (Decrease) increase in accrued expenses (854,274) 345,7551,156,598 (Decrease) increase in accrued rent 2,955,841 -- Increase in royalty advance - RPR (110,360) (1,340) (62,704) Decrease in other liabilities (2,125,604) (12,614,055) (22,132,051) Net cash used in operating activities Cash flows from investing activities: (387,020) (828,711)(4,434,179) Capital expenditures 861,521 41,600- Proceeds from sale of equipment - -(4,947,393) Increase in short-term investments - 4,947,39313,092,484 Proceeds from sale of short-term investments - -44,244 Decrease in long-term investments 305,315 - 673,600 Proceeds from cash surrender value of officer's life 779,816 4,160,282 4,428,756 insurance Net cash provided by investing activities 3,735,114 2,212,22118,601,558 Cash flows from financing activities: (17,798) (22,833) (19,770) Proceeds from issuance of common stock 3,717,316 2,189,388 18,581,788 Principal payments of obligations under capital leases Net cash provided by financing activities 2,371,528 (6,264,385)878,493 Net increase (decrease) in cash and cash equivalents 5,731,461 11,995,846 11,117,353 Cash and cash equivalents at beginning of period $8,102,989 $5,731,461 $11,995,846 Cash and cash equivalents at end of period
The accompanying notes are an integral part of these consolidated financial statements. F-7 ENZON, INC. AND SUBSIDIARIES Notes to Consolidated Financial Statements Years ended June 30, 1995, 1994 and 1993 (1) SUMMARY OF SIGNIFICANT ACCOUNTING POLICIES CONSOLIDATED FINANCIAL STATEMENTS The consolidated financial statements include the accounts of the Company and its wholly-owned subsidiaries. All intercompany transactions and balances are eliminated in consolidation. INVESTMENTS Cash equivalents include investments which consist primarily of debt securities and time deposits. The Company invests its excess cash in a portfolio of marketable securities of institutions with strong credit ratings and U.S. Government backed securities. The Company adopted the provisions of Statement of Financial Accounting Standards No. 115, "Accounting for Certain Investments in Debt and Equity Securities," (SFAS No. 115) on July 1, 1994. Under SFAS No. 115, the Company classifies its investment securities as held-to-maturity. Held- to-maturity securities are those securities which the Company has the ability and intent to hold to maturity. Held-to-maturity securities are recorded at cost which approximated the fair value of the investments at June 30, 1995. INVENTORY COSTING AND IDLE CAPACITY Inventories are stated at the lower of cost or market. Cost is determined by the first-in, first-out method and includes the cost of raw materials, labor and overhead. Costs associated with idle capacity at the Company's manufacturing facility are charged to cost of sales as incurred. Prior to the fourth quarter of the year ended June 30, 1994 and the approval of ONCASPAR, the Company's first FDA approved drug for a potentially large patient population, costs associated with idle capacity at the Company's manufacturing facility were charged to research and development expenses. PATENTS Patents related to the acquisition of Enzon Labs Inc., formerly Genex Corporation, were recorded at their fair value at the date of acquisition and are being amortized over the estimated useful lives of the patents. Accumulated amortization as of June 30, 1995 and 1994 was $588,000 and $428,000, respectively. Costs related to the filing of patent applications related to the Company's products and technology are expensed as incurred. PROPERTY AND EQUIPMENT Property and equipment are carried at cost. Depreciation is computed using the straight-line method. When assets are retired or otherwise disposed of, the cost and related accumulated depreciation are removed from the accounts, and any resulting gain or loss is recognized in operations for the period. The cost of repairs and maintenance is charged to operations as incurred; significant renewals and betterments are capitalized. F-8 REVENUE RECOGNITION Reimbursement from third party payors for ADAGEN is handled on an individual basis due to the high cost of treatment and limited patient population. Because of the uncertainty of reimbursement and the Company's commitment of supply to the patient regardless of whether or not the Company will be reimbursed, revenues for the sale of ADAGEN are recognized when reimbursement from third party payors becomes likely. Revenues from the sale of the Company's other products that are sold are recognized at the time of shipment and provision is made for estimated returns. Revenues related to programming services are recorded as sales when services are performed. Contract revenues are recorded as the earnings process is completed. Royalties under the Company's license agreement with Rhone-Poulenc Rorer Pharmaceuticals, Inc. ("RPR") (see note 10), related to the sale of ONCASPAR by RPR, are recognized when earned. RESEARCH AND DEVELOPMENT Research and development costs are expensed as incurred. CASH FLOW INFORMATION The Company considers all highly liquid securities with original maturities of three months or less to be cash equivalents. Cash payments for interest were approximately $4,000 in 1995, $5,000 in 1994, and $7,000 in 1993. There were no income tax payments made for the years ended June 30, 1995, 1994, and 1993. During the year ended June 30, 1995, the Company issued 100,000 shares of unregistered Common Stock in order to acquire an option to purchase the facility it currently leases in Piscataway, New Jersey. During the years ended June 30, 1994 and 1993, 8,000 and 14,000 shares of Series A Cumulative Convertible Preferred Stock were converted to 22,000 and 42,000 shares of Common Stock, respectively. Accrued dividends of $64,000 and $84,000 on the Series A Cumulative Convertible Preferred Stock that was converted were settled by issuing 7,000 and 10,000 shares of Common Stock and cash payments totalling $9 and $3 for fractional shares for the years ended June 30, 1994 and 1993, respectively. There was no conversion of the Series A Cumulative Convertible Preferred Stock during the year ended June 30, 1995. These transactions are non-cash financing activities. Management believes that its sources of liquidity will be sufficient to meet anticipated cash requirements through fiscal year end 1996. Upon exhaustion of these sources of liquidity, the Company's continued operations will depend on, among other things, its ability to realize significant revenues from the commercial sale of products, raise additional funds through equity or debt financing or obtain significant licensing, technology transfer or contract research and development fees. There can be no assurance that the Company will be able to obtain additional funding when it is needed or that such funding, if available, will be obtainable on terms favorable to the Company. F-9 NET LOSS PER COMMON SHARE Net loss per common share is based on net loss for the relevant period, adjusted for cumulative, undeclared preferred stock dividends of $218,000, $230,000 and $254,000 for the years ended June 30, 1995, 1994 and 1993, respectively, divided by the weighted average number of shares issued and outstanding during the period. Stock options, warrants and Common Stock issuable upon conversion of the preferred stock are not reflected as their effect would be antidilutive for both primary and fully diluted earnings per share computations. RECLASSIFICATIONS Certain prior year balances were reclassified to conform to the 1995 presentation. (2) RESTRUCTURING EXPENSE During the quarter ended March 31, 1995, the Company reduced its workforce by approximately 22 employees. As a result of these reductions, the Company was able to move its general and administrative operations into its existing research and development facility at 20 Kingsbridge Road in Piscataway, New Jersey. On March 31, 1995, the Company terminated its lease for 83,000 square feet at 40 Kingsbridge Road in Piscataway, New Jersey, its former general and administrative facility. As part of the termination agreement, the landlord was able to draw down on a $600,000 letter of credit that served as the security deposit for both buildings that the Company occupied on Kingsbridge Road in Piscataway. The termination payment, severance related to staff reductions, write-off of leasehold improvements, moving expenses and the commission due the Company's real estate broker related to the termination of the 40 Kingsbridge lease were recorded as a restructuring charge during the year ended June 30, 1995. Approximately $227,000 of the restructuring expense represents severance related to the staff reduction and the remaining $966,000 represents expenses incurred in conjunction with the lease termination. As part of the commission due the Company's real estate broker, 150,000 five-year warrants to purchase the Company's Common Stock at $2.50 per share were issued in August 1995. The termination of the Company's 40 Kingsbridge Road facility lease reduces the Company's future minimum lease payments by $650,000, $729,000 and $729,000 for the fiscal years ending June 30, 1996, 1997 and 1998, respectively, and an aggregate of $7,161,000 for the years thereafter. As of June 30, 1995, approximately $758,000 of the restructuring charge was unpaid and recorded in accrued expenses in the Consolidated Balance Sheet. The Company anticipates that the unpaid restructuring charge will be settled prior to December 31, 1995. (3) RELATED PARTY TRANSACTIONS The Company has license agreements with Research Corporation and its successor, Research Corporation Technologies, Inc. ("RCT"), related to the original PEG-Process patent. The PEG-Process was developed at Rutgers University in New Brunswick, New Jersey by Dr. Frank Davis, one of the Company's original founders, and two other inventors not affiliated with the Company. These agreements granted the Company an exclusive license to make, use and sell specific patented processes and products in countries in which a patent has been granted, or in which an application is pending, for the life of the patent. Under the terms of the agreements, the Company has the obligation to diligently develop, obtain regulatory approval for, and market these products. F-10 The Company is obligated under its agreement with RCT to pay a license maintenance fee of $75,000 each year during the term of this agreement, which shall be creditable by the Company against earned royalties payable, if any. As of June 30, 1995 and 1994, the Company had approximately $286,000 and $270,000 related to such agreements recorded as accrued expenses in the Consolidated Balance Sheets. During August 1992, the Company entered into a license agreement with two employees of the Company and an unrelated party to license a protein related technology. The Company paid $20,000 to each of the parties upon signing of the agreement and agreed to pay royalties of between 3% and 6% of net sales. The agreement also provides for a yearly maintenance fee of $15,000 commencing on January 30, 1993 and terminating on the first to occur of January 30, 1998 or the January 30th immediately preceding the date of the first sale of a licensed product. The agreement also requires aggregate minimum royalties of $25,000 beginning at the earlier of January 30, 1999 or the January 30th immediately following the date of the first sale of a licensed product and between $35,000 and $50,000 for subsequent years. The agreement terminates on the date on which the licensed patent having the latest expiration date expires, after accounting for extensions thereof. In both January 1995 and 1994, the Company paid yearly maintenance fees of $15,000. (4) COMMITMENTS AND CONTINGENCIES The Company has a long-term supply agreement for unmodified L- asparaginase, one of the raw materials used in ONCASPAR, under which the Company is required to purchase minimum quantities of this raw material on an annual basis. Under the agreement, which was amended during the fiscal year ended June 30, 1995, the Company is currently required to purchase $3,639,000 in raw material during the term of the contract, which expires on December 31, 1997. During the year ended June 30, 1995, the Company purchased approximately $186,000 related to this contract. The Company is required to purchase an additional $1,514,000 prior to December 31, 1995. The purchase requirements for the years ending December 31, 1996 and 1997 are $850,000 and $1,275,000, respectively. The Company has the option to satisfy $870,000 of the purchase requirement for the year ending December 31, 1995, without taking delivery of the product, by making a payment of $350,000. The Company has agreements with certain members of its upper management which provide for payments following a termination of employment occurring after a change in control of the Company. (5) INVENTORIES Inventories consist of the following: JUNE 30, 1995 1994 Raw materials $398,000 $407,000 Work in process 134,000 289,000 Finished goods 260,000 244,000 $792,000 $940,000 F-11 (6) PROPERTY AND EQUIPMENT Property and equipment consist of the following:
June 30, Estimated useful lives 1995 1994 USEFUL LIVES Equipment $9,284,000 $10,287,000 3-7 years Furniture and fixture 1,598,000 $1,845,000 7 years Vehicles 29,000 29,000 3 years Leasehold improvements 4,847,000 5,445,000 3-15 years $15,758,000 $17,606,000
Depreciation and amortization charged to operations, relating to property and equipment, were $2,317,000, $2,636,000 and $2,397,000 for the years ended June 30, 1995, 1994 and 1993, respectively. (7) STOCKHOLDERS' EQUITY SERIES A CUMULATIVE CONVERTIBLE PREFERRED STOCK The Company's Series A Cumulative Convertible Preferred Stock ("Series A Preferred Shares") is convertible into Common Stock at an annually increasing rate per share with a maximum conversion rate of $11 per share. As of June 30, 1995 and 1994, the conversion rates were $11 and $10 per share, respectively. The value of the Series A Preferred Shares for conversion purposes is $25 per share. Holders of the Series A Preferred Shares are entitled to an annual dividend of $2 per share, payable semiannually, but only when and if declared by the Board of Directors, out of funds legally available. Dividends on the Series A Preferred Shares are cumulative and accrue and accumulate but will not be paid, except in liquidation or upon conversion, until such time as the Board of Directors deems it appropriate in light of the Company's then current financial condition. No dividends are to be paid or set apart for payment on the Company's Common Stock, nor are any shares of Common Stock to be redeemed, retired or otherwise acquired for valuable consideration unless the Company has paid in full or made appropriate provision for the payment in full of all dividends which have then accumulated on the Series A Preferred Shares. Holders of the Series A Preferred Shares are entitled to one vote per share on matters to be voted upon by the stockholders of the Company. As of June 30, 1995 and 1994 undeclared accrued dividends in arrears were $1,149,000 or $10.54 per share and $931,000 or $8.54 per share, respectively. All common shares are of junior rank to the Series A Preferred Shares with respect to the preferences as to dividends, distributions and payments upon the liquidation, dissolution or winding up of the Company. F-12 During the years ended June 30, 1994 and 1993, 8,000 and 14,000 Series A Preferred Shares were converted to 22,000 and 42,000 shares of Common Stock. There were no conversions of Series A Preferred Shares during the year ended June 30, 1995. COMMON STOCK On January 22, 1993, the Company sold 3,175,000 shares of Common Stock in a public offering at a price of $6.50 per share, resulting in net proceeds to the Company of $18,484,000. On February 8, 1993, the stockholders voted to increase the number of authorized shares of Common Stock from 30,000,000 to 40,000,000. On February 1, 1994, an option to purchase 150,000 shares of the Company's Common Stock became exercisable. This option was granted to the Company's Chairman of the Board in 1989 and became exercisable upon the FDA's approval of ONCASPAR. The approval of ONCASPAR resulted in a non-cash compensation charge representing the difference between the exercise price of the option and the market value of the underlying Common Stock. On May 26, 1994, the Company sold 785,000 shares of Common Stock to Susquehanna Brokerage Services, Inc. ("Susquehanna") in a public shelf offering at a weighted average price of $2.55 per share, resulting in net proceeds to the Company of approximately $1,632,000. During the year ended June 30, 1995, the Company sold to Susquehanna, in a public shelf offering, an additional 954,000 shares of newly issued Common Stock. The shares were sold at a weighted average price of $2.06 per share, resulting in net proceeds to the Company of approximately $1,752,000. On January 5, 1995 the Company terminated its stock purchase agreement with Susquehanna. On April 1, 1995, the Company issued 100,000 shares of newly issued, unregistered Common Stock, valued at $2.25 per share, in consideration for an option to purchase the facility it currently leases in Piscataway, New Jersey. On June 30, 1995, in conjunction with the license of know-how related to PEG-INTRON A, the Company sold 847,000 shares of newly issued, unregistered Common Stock to Schering Corporation, resulting in net proceeds of approximately $1,983,000 (see note 10). Holders of shares of Common Stock are entitled to one vote per share on matters to be voted upon by the stockholders of the Company. As of June 30, 1995, the Company has reserved its common shares for special purposes as detailed below: F-13
Shares issuable upon conversion 248,000 of preferred stock Non-Qualified Stock Option Plan 4,477,000 Other options 200,000 4,925,000
SERIES A PREFERRED STOCK WARRANTS In connection with the private placement of the Series A Preferred Shares, the Company issued warrants to purchase 82,000 Series A Preferred Shares. Prior to the year ended June 30, 1995, 22,000 warrants were exercised. During the year ended June 30, 1995, the remaining warrants expired. ENZON LABS WARRANTS In connection with the acquisition of Enzon Labs Inc., the Company agreed to issue warrants to purchase 583,000 shares of Common Stock. Prior to the year ended June 30, 1995, 100 warrants were exercised. During the year ended June 30, 1995, the remaining warrants expired. (8) NON-QUALIFIED STOCK OPTION PLAN In November 1987, the Company's Board of Directors adopted a Non- Qualified Stock Option Plan (the "Plan"). On December 7, 1993, the stockholders voted to increase the number of shares reserved for issuance under the Plan from 4,000,000 to 5,000,000. Under the Plan, as amended, 4,477,000 shares of Common Stock as of June 30, 1995 are reserved for issuance pursuant to options which may be granted to employees, non- employee directors or consultants to the Company. The exercise price of the options must be at least 100% of the fair market value of the stock at the time the option is granted and an option may be exercised for a period of up to ten years from the date it is granted. The other terms and conditions of the options generally are to be determined by the Board of Directors, or an option committee appointed by the Board, at their discretion. A summary of the activity relating to the Plan follows:
Number of shares UNDER OPTION Outstanding at July 1, 1992 1,625,000 Granted at prices ranging from $4.25 to $9.00 467,000 Exercised at prices ranging from $3.75 to $4.38 (25,000) Cancelled at prices ranging from $6.00 to $11.50 (26,000) Outstanding at June 30, 1993 2,041,000
F-14
Granted at prices ranging from $2.38 to $6.00 1,292,000 Exercised at prices ranging from $3.75 to $4.88 (140,000) Cancelled at prices ranging from $4.00 to $14.88 (355,000) Outstanding at June 30, 1994 2,838,000 Granted at prices ranging from $1.88 to $3.13 1,412,000 Cancelled at prices ranging from $2.09 to $15.25 (645,000) Outstanding at June 30, 1995 3,605,000
At June 30, 1995, 2,257,000 options were exercisable at prices per share ranging from $2.00 to $14.88. On August 24, 1994, the Compensation Committee of the Board of Directors of the Company extended the exercise period of all outstanding five year options to ten years under the Plan. None of the options extended had exercise prices less than the fair market value of the Company's Common Stock on August 24, 1994, and accordingly, no compensation expense was recorded. (9) INCOME TAXES The Company adopted Statement of Financial Accounting Standards No. 109 (SFAS No. 109), "Accounting for Income Taxes" as of July 1, 1993. Under the asset and liability method of SFAS No. 109, deferred tax assets and liabilities are recognized for the estimated future tax consequences attributable to differences between financial statement carrying amounts of existing assets and liabilities and their respective tax bases. Deferred tax assets and liabilities are measured using enacted tax rates expected to apply to taxable income in the years in which those temporary differences are expected to be recovered or settled. Under SFAS No. 109, the effect on deferred tax assets and liabilities of a change in tax rates is recognized in income in the period that includes the enactment date. The effects of adopting SFAS No. 109 were not material to the financial statements at July 1, 1993. At June 30, 1995 and 1994, the tax effects of temporary differences that give rise to the deferred tax assets and deferred tax liabilities are as follows: 1995 1994 Deferred tax assets: Inventories $57,000 $450,000 Investment valuation reserve 86,000 86,000 Contribution carryover 10,000 9,000 Compensated absences 103,000 138,000 Excess of financial statement over tax depreciation146,000 - Royalty advance - RPR 1,340,000 - Sanofi liability 524,000 524,000 Non-deductible expenses 457,000 424,000 Federal and state net operating loss carryforwards35,816,000 35,054,000 Research and development and investment tax credit carryforwards5,770,000 5,688,000 F-15 Total gross deferred tax assets 44,309,000 42,373,000 Less valuation allowance (43,597,000) (41,410,000) Net deferred tax assets 712,000 963,000 Deferred tax liabilities: Excess of tax over financial statement depreciation - (231,000) Step up in basis of assets related to acquisition of Enzon Labs Inc. (712,000) (732,000) Total gross deferred tax liabilities (712,000) (963,000) Net deferred tax $0 $0 A valuation allowance is provided when it is more likely than not that some portion or all of the deferred tax assets will not be realized. The valuation allowance for deferred tax assets as of July 1, 1993 was $34,053,000. The net change in the total valuation allowance for the years ended June 30, 1995 and 1994 were increases of $2,187,000 and $7,357,000, respectively. Subsequently recognized tax benefits for the years ended June 30, 1995 and 1994 of $940,000 and $1,025,000 relating to the valuation allowance for deferred tax assets will be allocated to additional paid-in capital. At June 30, 1995, the Company had federal net operating loss carryforwards of approximately $90,627,000 for tax reporting purposes, which expire in the years 1997 to 2010. The Company also has investment tax credit carryforwards of approximately $30,000 and research and development tax credit carryforwards of approximately $5,740,000 for tax reporting purposes which expire in the years 1998 to 2010. As part of the Company's acquisition of Enzon Labs Inc., the Company acquired the net operating loss carryforwards of Enzon Labs Inc. of $67,949,000 which expire between October 31, 1994 and October 31, 2006. As a result of the change in ownership the utilization of these carryforwards is limited to $613,000 per year. (10) SIGNIFICANT AGREEMENTS RHONE-POULENC RORER AGREEMENT The Company has granted RPR an exclusive license ("the License Agreement") in the United States to sell ONCASPAR, and any other PEG- asparaginase product (the "Product") developed by Enzon or RPR during the term of the License Agreement. Under this agreement, Enzon was entitled to licensing payments totaling $6,000,000, of which $500,000 and $5,500,000 were paid during the fiscal years ended June 30, 1995 and 1994, respectively. F-16 During January 1995, the Company amended its exclusive U.S. marketing rights license with RPR for ONCASPAR. Under the amended agreement, Enzon will earn a base royalty of 10% for the year ending December 31, 1995 and 23.5% thereafter, until 2008, on net sales of ONCASPAR up to agreed upon amounts, as opposed to 50% of net profits provided for under the original agreement. Additionally, Enzon will earn a super royalty of 23.5% for the year ending December 31, 1995 and 43.5% thereafter, until 2008 on net sales of ONCASPAR which exceed the agreed upon amounts, with the limitation that the total royalties earned for any such year shall not exceed 33% of net sales. The amendment eliminates RPR's requirement to make certain minimum advertising, promotional and clinical expenditures. Future decisions regarding clinical development will be at RPR's discretion. The amended agreement also provides for a payment of $3,500,000 in advance royalties, which was received in January 1995. Base royalties due under the amended agreement will be offset against a credit of $5,970,000 (which represents the royalty advance plus reimbursement of certain amounts due to RPR under the previous agreement and interest expense) before cash payments for base royalties will be made. Super royalties will be paid to the Company when earned. The royalty advance is shown as a long term liability, with the corresponding current portion included in accrued expenses on the Consolidated Balance Sheet as of June 30, 1995. The royalty advance will be reduced as base royalties are recognized under the agreement. The agreement prohibits RPR from selling a competing PEG-asparaginase product anywhere in the world during the term of the License Agreement and for five years thereafter. The revised License Agreement terminates in December 2008, subject to early termination by either party due to a default by the other or by RPR at any time on one year's prior notice to Enzon. Upon any termination all rights under the License Agreement revert to Enzon. The Company has also granted exclusive licenses to sell ONCASPAR in Canada and Mexico to RPR. These agreements provide for RPR to obtain marketing approval of ONCASPAR in Canada and Mexico and for the Company to receive royalties on sales of ONCASPAR in these countries, if any. The Company is currently pursuing other licenses for marketing and distribution rights for ONCASPAR outside North America. A separate supply agreement with RPR requires RPR to purchase from Enzon all of RPR's requirements for the Product for sales in North America. SANOFI WINTHROP AGREEMENT In June 1989, the Company, Sanofi Winthrop, Inc. ("Sanofi"), formerly Sterling Winthrop, Inc. and Eastman Kodak Company ("Kodak") signed a license agreement (the "Sanofi Agreement") which supersedes the Company's March 1987 license agreement with Kodak (the "Kodak License Agreement"). Sterling Winthrop, Inc., a subsidiary of Kodak, was sold in 1994 to Sanofi Pharmaceuticals. The Company received $5,000,000 and $2,000,000 under the Sanofi Agreement during the years ended June 30, 1989 and 1990, respectively, and transferred to Sanofi all responsibilities for development and regulatory approval in the United States for PEG- superoxide dismutase ("PEG-SOD") and certain technological know-how for the product. All future development and regulatory approval costs for PEG-SOD, including the cost of unmodified enzymes for the product used in pre-approval testing, will be borne by Sanofi. F-17 Under the agreement, Sanofi has the exclusive worldwide marketing rights, foreign regulatory approval responsibility and foreign manufacturing rights for PEG-SOD. Generally, the Company will be entitled to 40% of the net profits from sales of PEG-SOD in the United States during the life of the basic U.S. patent covering the product, with agreed-upon limits on the amount of expenses that can be deducted by Sanofi from revenues, if any, before calculating the profit split. Under the Sanofi Agreement, Enzon is entitled to manufacture PEG-SOD for United States sales by Sanofi; however, Sanofi has the right to take over such manufacturing or have such manufacturing performed on its behalf in consideration for the payment, under certain circumstances, of an additional royalty. Sanofi is manufacturing the PEG-SOD utilized in its clinical trials and the Company expects that Sanofi will manufacture the product for U.S. sales if it is approved by the FDA. The Sanofi Agreement terminates on a country by country basis upon the expiration of the last to expire of the patents licensed to the Company under its License Agreement with RCT. The United States patent licensed to Enzon under the RCT Agreement expires in December 1996. The Company has entered into an agreement with RCT to extend this patent for up to five years. Upon such patent expiration or termination of the Sanofi Agreement due to the Company's breach of the agreement or bankruptcy, the license granted to Sanofi automatically converts to a non-exclusive, royalty-free, paid-up license, except that Sanofi may maintain an exclusive license with respect to PEG-SOD by paying the Company a reduced royalty on Sanofi's sales of PEG-SOD. Sanofi has the right to terminate the Sanofi Agreement at any time with respect to any or all of the countries which are covered by the agreement with no further obligation to the Company, in which case all rights terminated by Sanofi in this manner shall revert to the Company. Under the original Kodak License Agreement signed in March 1987, the Company issued 2,000,000 shares of its Common Stock to Kodak for a cash payment of $6,000,000. The Company also received $9,000,000 under this agreement to fund all activities to obtain FDA approval of PEG-SOD. The Sanofi Agreement requires a credit to Sanofi (the "shortfall") for monies not expended for the development of PEG-SOD under the Kodak Agreement. The shortfall balance as of June 30, 1995 and 1994, was $1,313,000, and is shown as a current liability in the Consolidated Balance Sheets. The shortfall may be applied by Sanofi as a credit against amounts owed the Company by Sanofi for clinical supplies. Sanofi has notified the Company that it does not require future clinical supplies from the Company and, therefore, the Company has no further obligation under the agreement to supply PEG-SOD to Sanofi. SCHERING AGREEMENT In November 1990, Enzon and Schering Corporation ("Schering") signed an agreement (the "Schering Agreement") to apply the PEG Process to Schering's INTRON A (interferon alfa 2b), a genetically-engineered anticancer and antiviral drug. In August 1992, a Phase I human clinical trial began using PEG-INTRON A for the indication of hepatitis. The protocol for that trial has been completed. Schering and Enzon amended the Schering Agreement to develop a PEG-INTRON A formulation having improved performance characteristics. Enzon has prepared and delivered clinical batches of the new PEG-INTRON A formulations to Schering for additional clinical trials. F-18 On June 30, 1995, the Company and Schering further amended the Schering Agreement pursuant to which Enzon agreed to transfer proprietary know-how and manufacturing rights for PEG-INTRON A to Schering for $3,000,000, of which $2,000,000 was paid on June 30, 1995 and $1,000,000 will be paid upon completion of the know-how transfer, as defined in such amended agreements. In connection with the amendment, the Company also sold to Schering 847,000 shares of unregistered, newly issued Common Stock for $2,000,000 in gross proceeds. Under the current Schering Agreement, Enzon retained an option to become Schering's exclusive manufacturer of PEG-INTRON A for the United States market upon FDA approval of such product. Under the Schering Agreement, Enzon is entitled to receive sequential payments, totalling approximately $6,000,000, subject to the achievement of certain milestones in the product's development program, as well as payments for the clinical material it produces. During the year ended June 30, 1992, the Company received the first milestone payment of $450,000 related to the filing of an Investigational New Drug Application. The Company will also receive royalties on worldwide sales of PEG-INTRON A, if any. Schering will be responsible for conducting and funding the clinical studies, obtaining regulatory approval and marketing the product worldwide on an exclusive basis. The Schering Agreement terminates, on a country-by-country basis, upon the expiration of the last to expire of any future patents covering the product which may be issued to Enzon, or 15 years after the product is approved for commercial sale, whichever shall be the later to occur. This agreement is subject to Schering's right of early termination if the product does not meet specifications, or if Enzon fails to obtain or maintain the requisite product liability insurance, or if Schering makes certain payments to Enzon. If Schering terminates the agreement because the product does not meet specifications, Enzon may be required to refund certain of the milestone payments. BAXTER AGREEMENT In November 1992, Enzon and Baxter Healthcare Corporation ("Baxter") signed an agreement granting Baxter a non-exclusive worldwide license to Enzon's SCA protein technology. It is anticipated that Baxter's biotech group will use the SCA proteins in its cancer research programs focusing on human stem cell isolation and gene therapy. Under the agreement, the Company received $350,000 during the year ended June 30, 1993 for the execution of the agreement and is entitled to additional sequential payments, subject to the achievement of certain milestones in the products' development of $500,000 for each product developed up to a maximum of $2,500,000. Baxter will have the exclusive worldwide rights to manufacture and market any products which it develops and Enzon will receive certain royalties on Baxter's sales, if any. ELI LILLY (HYBRITECH) AGREEMENT In December 1992, Enzon and Hybritech Incorporated ("Hybritech"), a subsidiary of Eli Lilly & Co., signed an agreement granting Hybritech a non-exclusive worldwide license to Enzon's SCA protein technology. Under the agreement, Enzon is entitled to certain upfront payments totalling $1,200,000, of which $700,000 and $500,000 were received during the years ended June 30, 1994 and 1993, respectively, and will receive certain royalties on Hybritech sales of products, if any, that may be developed using Enzon's SCA protein technology. F-19 BRISTOL-MYERS SQUIBB In September 1993, the Company and Bristol-Myers Squibb ("Bristol-Myers") signed a license agreement for Enzon's SCA protein technology granting Bristol-Myers a worldwide, semi-exclusive license for a particular antigen. Under the agreement, Enzon is entitled to receive certain upfront payments and sequential payments, subject to the achievement of certain milestones in the development program. Bristol-Myers will have the right to manufacture and market products which it develops and Enzon will receive certain royalties on Bristol-Myers sales, if any. Enzon also granted Bristol-Myers options to take non-exclusive licenses under patent rights for other applications/fields for certain additional payments. During the year ended June 30, 1994, Enzon received $200,000 under this agreement. In July 1994, Bristol-Myers paid $1,800,000 to Enzon and exercised its option to acquire a worldwide non-exclusive license for SCA protein technology. The non-exclusive license is for all areas of drug development. (11) LEASES The Company has several leases for office, warehouse, production and research facilities and equipment. Future minimum lease payments, net of subleases, for noncancellable operating leases (with initial or remaining lease terms in excess of one year) and the present value of future minimum capital lease payments as of June 30, 1995 are: Year ending Capital Operating JUNE 30, LEASES LEASES 1996 $2,000 $1,592,000 1997 2,000 1,699,000 1998 2,000 1,710,000 1999 - 1,130,000 2000 - 497,000 Later years, through 2007 - 3,878,000 Total minimum lease payments$6,000 $10,506,000 Rent expense amounted to $1,642,000, $2,181,000 and $2,469,000 for the years ended June 30, 1995, 1994 and 1993, respectively. The Company currently subleases a portion of two of its facilities. For the years ended June 30, 1995 and 1994, rent expense is net of subrental income of $353,000 and $101,000, respectively. There were no subleases in the year ended June 30, 1993. (12) CASH SURRENDER VALUE OF LIFE INSURANCE As of June 30, 1995, the Company maintains a split-dollar life insurance for its Chairman of the Board with a face value of $3,000,000. Under the split-dollar agreement, in the event of death, the Company will receive the greater of the cash accumulation value or the premiums paid. The remainder of the death benefit, as defined, paid by the insurance company, will be paid to the named beneficiaries of the insured. The Company also maintains key man life insurance policies with a face value of $1,000,000 on both the President and Chief Executive Officer and the Chairman of the Board. F-20 In July 1992, the Company took a loan against the split dollar life insurance policy for $674,000. At June 30, 1995 and 1994, the cash surrender value of $847,000 and $1,155,000, respectively, less the outstanding loan balance and accrued interest of $847,000 and $782,000, respectively, is recorded in other assets in the Consolidated Balance Sheets. During the year ended June 30, 1995, the Company cancelled a separate single premium key man life insurance policy on its Chairman of the Board and received the cash surrender value of $305,000. (13) RETIREMENT PLANS The Company maintains a defined contribution, 401(k), pension plan for substantially all its employees. Effective July 1, 1991, the Company revised the plan to provide for a match of employee contributions to the plan. The Company matches 25% of the employee's contribution up to 6% of compensation, as defined. Effective, January 1, 1995, the Company's match is invested solely in a fund which purchases the Company's Common Stock in the open market. Total Company contributions for the years ended June 30, 1995, 1994 and 1993 were $80,000, $94,000 and $93,000, respectively. (14) ACCRUED EXPENSES Accrued expenses consist of: JUNE 30, 1995 1994 Accrued wages and vacation $398,000 $1,260,000 Reserve for product returns 298,000 600,000 Accrued employee medical claims278,000 537,000 Accrued Medicaid rebates 813,000 435,000 Accrued restructuring costs 758,000 - Current portion of royalty advance - RPR 400,000 - Other 1,100,000 1,406,000 $4,045,000 $4,238,000 (15) FOURTH QUARTER INFORMATION During the fourth quarter of the year ended June 30, 1994, the Company recorded a charge to operations for excess raw material (PEG) of $618,000. (16) SALES INFORMATION During the years ended June 30, 1995, 1994 and 1993, the Company had export sales of $2,105,000, $2,085,000, and $1,631,000, respectively. Sales to Europe represented $1,841,000, $1,957,000 and $1,346,000 during the years ended June 30, 1995, 1994 and 1993, respectively. Approximately 42%, 28% and 15% of the Company's ADAGEN sales for the years ended June 30, 1995, 1994 and 1993, respectively, were made to Medicaid patients. (17) OTHER INCOME During the year ended June 30, 1995, the Company received approximately $645,000 for an insurance settlement related to ADAGEN that was destroyed in shipment. F-21 EXHIBIT INDEX Exhibit Page NUMBERS DESCRIPTION NUMBER 10.17 Amendment to Employment Agreement with Peter G. Tombros dated as of May 15, 1995 E1 21.0 Subsidiaries of Registrant E2 23.0 Consent of KPMG Peat Marwick LLP E3 23.1 Consent of Lerner, David, Littenberg, Krumholz & MentlikE4

As of May 15, 1995


Mr. Peter G. Tombros
159 Lambert Road
New Canaan, CT  06840


      Re:  AMENDMENT TO EMPLOYMENT AGREEMENT

Dear Peter:

      This  letter  agreement, when signed  by  you,  will  serve  as  a  first
amendment to your employment  agreement  with Enzon, Inc. (the "Company") dated
as of March 25, 1994 (the "Employment Agreement").

      Pursuant to Section 3(b) of the Employment Agreement, you are entitled to
receive an award (the "Award") under the Company's  Total  Compensation Program
for Officers and Senior Executives (the "Program") based on  the  completion of
your  first  year  of  employment  with  the Company.  The Employment Agreement
further provides that the Award is to consist  of  an  option granted under the
Company's  Non-Qualified  Stock Option Plan (the "Plan") and  cash  having  the
value and based on the terms set forth therein.

      This will confirm our  agreement  that you will not receive the Award for
the completion of your first year of employment with the Company as provided in
Section 3(b) of the Employment Agreement,  and  in  lieu  thereof,  the Company
shall  grant to you an option (the "Option") under the Plan to purchase  84,000
shares of the Company's common stock, $.01 par value (the "Common Stock").  The
exercise  price  per  share  of  Common Stock shall be $2.00, which is the fair
market value of a share of Common  Stock  on the date hereof.  The Option shall
be exercisable as to 42,000 shares on May 15,  1996  and  as  to  the remaining
42,000  shares on May 15, 1997 and shall terminate in its entirety on  May  15,
2005.  The  Option  is  not  being  granted pursuant to the Program.  Except as
provided herein, the Employment Agreement shall remain unchanged.

      To  evidence your agreement to the  foregoing,  kindly  countersign  this
letter on the line provided below.


                                          Very truly yours,

                                          ENZON, INC.
                                          By:/S/ KENNETH J. ZUERBLIS
                                          Name: Kenneth J. Zuerblis
                                          Title: Vice President, Finance


AGREED AND ACCEPTED


/S/ PETER G. TOMBROS
Peter G. Tombros



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                          SUBSIDIARIES OF REGISTRANT




Symvex Inc.  is a wholly-owned subsidiary of the Registrant incorporated in the
State of Delaware.  Symvex Inc.  did business under its own name.

Enzon Labs Inc., is a wholly-owned subsidiary of the Registrant incorporated in
the State of Delaware.  Enzon Labs Inc. does business under its own name.

Enzon Pharm. B.V.  is  a wholly-owned subsidiary of the Registrant incorporated
in the Netherlands.

Enzon GmbH is a wholly-owned  subsidiary  of  the  Registrant  incorporated  in
Germany.







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INDEPENDENT AUDITORS' CONSENT




The Board of Directors
Enzon Inc.:

We  consent to incorporation by reference in the Registration Statement No. 33-
50904  on  Form  S-8  of  Enzon,  Inc.  of our report dated September 21, 1995,
relating to the consolidated balance sheets  of Enzon, Inc. and subsidiaries as
of  June  30,  1995  and  1994,  and  the  related consolidated  statements  of
operations, stockholders' equity, and cash flows  for  each of the years in the
three-year period ended June 30, 1995, which report appears  in  the  June  30,
1995 annual report on Form 10-K of Enzon, Inc.






                                    /S/KPMG PEAT MARWICK LLP
                                    KPMG Peat Marwick LLP




New York, New York
September 27, 1995




                                                       E3


                              CONSENT OF COUNSEL


      We  hereby  consent  to  the  reference  to  our  firm  under the caption
"Business - Patents" in the Annual Report on Form 10-K of Enzon,  Inc.  for the
fiscal year ended June 30, 1995.



                              /S/LERNER, DAVID, LITTENBERG,
                                    KRUMHOLZ & MENTLIK
September 22, 1995            Lerner, David, Littenberg,
                                         Krumholz & Mentlik








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