
                                                                       EXHIBIT 1


     SOUTH SAN FRANCISCO, Calif. & BERKELEY, Calif.--(BUSINESS WIRE)--Sept. 9,
2003--Genentech, Inc. (NYSE:DNA) and XOMA Ltd. (Nasdaq:XOMA) today announced
that the U.S. Food and Drug Administration's (FDA) Dermatologic and Ophthalmic
Drug Advisory Committee (DODAC) voted unanimously (11-0) to recommend that
Raptiva(TM) (Efalizumab) be approved for the treatment of moderate-to-severe
plaque psoriasis in adults age 18 or older.

     Although the FDA is not bound by the recommendations of its advisory
committees, it generally follows their advice. Genentech and XOMA will continue
discussions with the FDA regarding product labeling and post-marketing
commitments.

     "Today's advisory committee recommendation is an important step toward
providing a new therapeutic option for people with psoriasis," said Hal Barron,
M.D., F.A.C.C., Genentech's vice president, Medical Affairs. "People with
psoriasis are faced with a lifetime of disease management. If approved, Raptiva
may offer patients a new approach to control of this chronic disease."

     Raptiva is a T-cell modulator designed to selectively and reversibly block
the activation of T-cells that cause psoriasis. In clinical trials, Raptiva
demonstrated rapid onset of action in the reduction of symptoms associated with
psoriasis, including a reduction in the thickness, scaling and redness of skin
lesions, or plaques. The therapy was administered once weekly via subcutaneous
injection, and in several of the trials, was self-administered by patients at
home.

     Jack Castello, XOMA's president and chief executive officer added, "We are
pleased with the FDA advisory committee's unanimous recommendation and if
Raptiva is approved, we look forward to offering an effective biologic treatment
option to patients who desire to manage their disease and remove the limitations
psoriasis currently imposes on their lives."

     Raptiva is being developed by Genentech and XOMA in the United States. The
Biologics License Application (BLA) for Raptiva was filed in December 2002, with
a supplemental data amendment filing in May 2003. An FDA response on the Raptiva
BLA is expected by October 27, 2003.

     Genentech and XOMA are collaborating on the development and
commercialization of Raptiva in the United States. Serono S.A., Genentech's
marketing partner outside the United States and Japan, announced in February
2003 that it had submitted a Marketing Authorization Application (MAA) to the
European Agency for the Evaluation of Medicinal Products (EMEA) for European
Union Approval of Raptiva in psoriasis. Serono has also submitted Raptiva data
for marketing approval in Canada, Switzerland, Australia and New Zealand and is
filing in additional countries.

     Raptiva Phase III Clinical Trials Results

     The FDA advisory committee's recommendation was based on data from four
randomized, placebo-controlled Phase III studies. The FDA submission (BLA)
included data on more than 2,700 patients treated with Raptiva, representing the
largest existing database of patients treated with a biologic therapy for
psoriasis. The Phase III trials were designed to evaluate the safety and
efficacy of Raptiva as a potential treatment for moderate-to-severe plaque
psoriasis.


The studies had a primary efficacy endpoint of 75 on the Psoriasis
Area and Severity Index (PASI), measuring the proportion of patients achieving a
75 percent or greater PASI score improvement. The PASI score is a rating system
that incorporates thickness of psoriatic plaque, degree of scaling, level of
redness, and percentage of body surface affected. Secondary endpoints for the
Phase III studies included physician assessment, patient-reported outcomes and
quality-of-life improvements.

     Data presented at today's DODAC advisory committee hearing included
efficacy data for 12 and 24 weeks of treatment.

     --   At week 12 of the pivotal, randomized, double blind,
          placebo-controlled Phase III study, 27 percent (98/369) of the
          patients receiving Raptiva achieved PASI 75 and 59 percent (216/369)
          of patients achieved a 50 percent or greater PASI improvement (PASI
          50).

     --   At 24 weeks of the open-label, extended treatment period following the
          first 12 weeks of treatment, 44 percent (161/369) of patients who had
          received at least one dose of Raptiva during the first 12 weeks
          achieved PASI 75 and 66 percent (245/369) of patients achieved PASI
          50.

     Raptiva was well tolerated in Phase III studies. Adverse events that
occurred in at least five percent of patients treated with Raptiva and one
percent more frequently than in the placebo group included headache, chills,
pain, flu syndrome, fever, asthenia, nausea, myalgia (muscle pain), and
pharyngitis. Five of these events (headache, chills, fever, nausea and myalgia)
were predominantly acute adverse events, principally seen following the first
two injections of Raptiva. For the third and subsequent doses, the incidence of
acute adverse events was similar between the Raptiva and placebo groups. Less
than three percent of patients were discontinued from treatment due to adverse
events. Infrequent serious adverse events included psoriatic reccurances (most
of which occured after treatment was stopped), thrombocytopenia and infection.

     If approved, the final efficacy and safety description included in
Raptiva's product labeling will be determined by the FDA.

About Psoriasis


     Psoriasis occurs when new skin cell growth rapidly accelerates, resulting
in thick, red, scaly, inflamed patches on the skin surface. Psoriasis affects
approximately 4.5 million Americans. Plaque psoriasis, the most common form of
the disease, is characterized by inflamed patches of skin ("lesions") topped
with silvery white scales. Psoriasis can be limited to a few spots or involve
extensive areas of the body, appearing most commonly on the scalp, knees, elbows
and trunk. Although it is highly visible, psoriasis is not a contagious disease.
While there are a number of medications that may help control the symptoms of
psoriasis, there is currently no cure.


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About Genentech


     Genentech is a leading biotechnology company that discovers, develops,
manufactures and commercializes biotherapeutics for significant unmet medical
needs. Sixteen of the currently approved biotechnology products originated from
or are based on Genentech science. Genentech manufactures and commercializes 11
biotechnology products in the United States. The company has headquarters in
South San Francisco, California and is traded on the New York Stock Exchange
under the symbol DNA. For additional information about the company, please visit
http://www.gene.com.

     Immediately following the advisory committee meeting, Genentech will host a
webcast to discuss the results of the meeting. The webcast began at 3:00 p.m.
Pacific Time/6:00 p.m. Eastern Time on September 9, 2003. The live webcast can
be accessed by going to Genentech's website at http://www.gene.com and will be
archived and available for replay until 5:00 p.m. Pacific Time on September 16,
2003.

     An audio replay of the webcast will be available beginning at 5:00 p.m.
Pacific Time/8:00 p.m. Eastern Time on September 9, 2003 and ending at 5:00 p.m.
Pacific Time/8:00 p.m. Eastern Time on September 16, 2003. Access numbers for
this replay are: 1-800-642-1687 (U.S./Canada) and 1-706-645-9291
(international); passcode number is 2287750.

About XOMA


     XOMA develops and manufactures antibody and other protein-based
biopharmaceuticals for disease targets that include immunological and
inflammatory disorders, cancer and infectious diseases. XOMA's programs include
collaborations: with Genentech, Inc. on the Raptiva(TM) antibody for psoriasis
(BLA submission), psoriatic arthritis (Phase II) and other indications; and with
Millennium Pharmaceuticals, Inc. on two biotherapeutic agents, CAB-2 and
MLN2201, for vascular inflammation indications (preclinical and phase I,
respectively). Earlier-stage development programs focus on antibodies and other
compounds developed by XOMA for the treatment of cancer, retinopathies and acne.
For more information about XOMA's pipeline and activities, please visit XOMA's
website at http://www.xoma.com/.

Regarding XOMA:


     Statements made in this news release related to the BLA review and other
aspects of the regulatory process, as well as the collaborative arrangements
regarding Raptiva(TM), or that otherwise relate to future periods, are forward
looking statements within the meaning of Section 27A of the Securities Act of
1933 and Section 21E of the Securities Exchange Act of 1934. These statements
are based on assumptions that may not prove accurate. Actual results could
differ materially from those anticipated due to certain risks inherent in the
biotechnology industry and for companies engaged in the development of new
products in a regulated market. These risks include those related to safety and
efficacy of the product being studied (including the product's ability to remain
safe and efficacious in the long term); action, inaction or delay by the Food
and Drug Administration, European regulators and/or their advisory bodies;
analysis and


                                      -3-

interpretation by these entities and others of scientific data; failure of the
FDA to follow the recommendation of the DODAC; changes in the status of existing
collaborative relationships; the ability of collaborators to meet their
obligations; and market demand for products. These risks are discussed in XOMA's
most recent annual report on Form 10-K and in other SEC filings. Consider such
risks carefully in evaluating XOMA's prospects.

CONTACT:  Genentech
          Tara Cooper, 650-225-5505 (Media)
          Kathee Littrell, 650-225-1034 (Investors)
          or
          XOMA
          Laura Zobkiw, 510-204-7273


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