Pursuant to Rule 425

Filed by Cell Therapeutics, Inc.

Pursuant to Rule 425 under the Securities Act of 1933

And deemed filed pursuant to Rule 14a-12

Of the Securities and Exchange Act of 1934

Subject Company: Cell Therapeutics, Inc.

Commission File No: 001-12465

 

The following is the entire presentation given by Cell Therapeutics, Inc. at its annual meeting of stockholders, held on June 20, 2003.

 

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Welcome

 

Shareholders & Guests

 

June 20, 2003

 

1

 

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Annual Shareholders Meeting

 

James A. Bianco    

President and CEO

(GRAPHIC)

 

We’re fighting cancer

 

2

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Business Meeting Agenda

 

  Approve minutes
  Elect Directors
  Approve 2003 Equity Incentive Plan
  Approve an amendment to Employee Stock Purchase Plan
  Ratify selection of E&Y as independent auditors

 

3

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Business Meeting

 

  Call meeting to order
  Introduction of officers, directors, accountants, inspector of elections
  Record Date: May 7, 2003
  Confirmation of quorum established

 

4

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Business Meeting

 

  Approval of minutes

 

5

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Business Meeting

 

  Election of class III Directors
-   Mary Mundinger
-   Jack Singer
-   Marty Sutter
  Election of class I Director
-   John Fluke

 

6

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Business Meeting

 

  Approve 2003 Equity Incentive Plan

 

7

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Business Meeting

 

  Approve amendment to the Company’s 1996 Employee Stock Purchase Plan to increase the number of shares by 150,000 to a total of approximately 635,000 shares

 

8

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Business Meeting

 

  Ratify selection of Ernst & Young as independent auditors
  Open the floor to motions

 

9

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Business Meeting

 

  Voting
  Results of voting
  Conclusion of the business items

 

10

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Management Presentation

 

[GRAHIC]

 

11

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Agenda

 

  Oncology Portfolio Strategy J. Bianco
  Market Dynamics
  -   Hematology Market
  -   Solid Tumor Market
  CTI-Novuspharma merger
  Commercial Development E. Kenney
  Research and Clinical Development J. Singer
  Closing Remarks J. Bianco

 

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Forward Looking Statement

 

This presentation contains forward-looking statements within the meaning of the “safe harbor” provisions of the Private Securities Litigation Reform Act of 1995. These statements are based on management’s current expectations and beliefs and are subject to a number of factors and uncertainties that could cause actual results to differ materially from those described in the forward-looking statements. The forward-looking statements contained in this presentation include statements about future financial and operating results, the proposed CTI/Novuspharma merger, and risk and uncertainties that could affect CTI’s product and products under development. These statements are not guarantees of future performance, involve certain risks, uncertainties and assumptions that are difficult to predict, and are based upon assumptions as to future events that may not prove accurate. Therefore, actual outcomes and results may differ materially from what is expressed herein. For example, if either of the companies do not receive required stockholder approvals or fail to satisfy other conditions to closing, the transaction will not be consummated. In any forward-looking statement in which CTI expresses an expectation or belief as to future results, such expectation or belief is expressed in good faith and believed to have a reasonable basis, but there can be no assurance that the statement or expectation or belief will result or be achieved or accomplished. The following factors, among others, could cause actual results to differ materially from those described in the forward-looking statements: risks associated with preclinical, clinical and sales and marketing developments in the biopharmaceutical industry in general and in particular including, without limitation, the potential failure to meet TRISENOX® revenue goals, the potential failure of XYOTAX to prove safe and effective for treatment of non-small cell lung and ovarian cancers, the potential failure of TRISENOX® to continue to be safe and effective for cancer patients, determinations by regulatory, patent and administrative governmental authorities, competitive factors, technological developments, costs of developing, producing and selling TRISENOX® and CTI’s products under development in addition to the risk that the CTI and Novuspharma businesses will not be integrated successfully; costs related to the proposed merger, failure of the CTI or Novuspharma stockholders to approve the proposed merger; and other economic, business, competitive, and/or regulatory factors affecting CTI’s and Novuspharma’s businesses generally, including those set forth in CTI’s filings with the SEC, including its Annual Report on Form 10-K for its most recent fiscal year and its most recent Quarterly Report on Form 10-Q, especially in the “Factors Affecting Our Operating Results” and “Management’s Discussion and Analysis of Financial Condition and Results of Operations” sections, and its Current Reports on Form 8-K. CTI is under no obligation to (and expressly disclaims any such obligation to) update or alter its forward-looking statements whether as a result of new information, future events, or otherwise.

 

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Where You Can Find

Additional Information

 

Cell Therapeutics, Inc. (CTI) will file a proxy statement/prospectus and other documents concerning the proposed merger transaction with the Securities and Exchange Commission (SEC). Investors and security holders are urged to read the proxy statement/prospectus when it becomes available and other relevant documents filed with the SEC because they will contain important information. Security holders may obtain a free copy of the proxy statement/prospects (when it is available) and other documents filed by CTI with the SEC at the SEC’s website at http://www.sec.gov. The proxy statement/prospectus and these other documents may also be obtained for free from CTI, Investor Relations: 501 Elliott Avenue West, Suite 400 Seattle, WA 98119, www.cticseattle.com.

 

CTI and Novuspharma S.p.A. and their respective directors and executive officers and other members of their management and their employees may be deemed to be participants in the solicitation of proxies from the shareholders of CTI and Novuspharma with respect to the transactions contemplated by the merger agreement. Information about the directors and officers of CTI is included in CTI’s Proxy Statement for its 2003 Annual Meeting of Stockholders filed with the SEC on May 14, 2003.

 

This document is available free of charge at the SEC’s website at http://www.sec.gov and from CTI.

 

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Making Cancer More Treatable

 

Providing less toxic, more effective

therapies to treat and cure cancer while

permitting patients and their families to

maintain their dignity and quality of life

 

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New Paradigm in Treating Cancer

 

Improving treatment outcomes – four strategic directions

 

  Improving tolerability of existing chemotherapy agents
  Combining therapies to work more effectively without increased side effects
  Developing tumor targeted therapies exploiting human genome
  Treating cancer as a chronic disease without impacting quality of life

 

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Oncology Strategy

 

  Improve the safety and efficacy of existing agents which provide the cornerstone for standard of care
  -   Taxanes (>$2B)                       XYOTAX
  -   Camptothecins (>$1B)             CT-2106
  -   Anthracyclines (>$500M)        Pixantrone

 

  Develop new agents with unique mechanisms of tumor cell killing without more side effects
  -   TRISENOX®
  -   LPAAT-ß inhibitors

 

  Develop significant sales and marketing presence in cancer market segments where leverage is possible
  -   Blood-related cancer market

 

  Consider co-marketing relationship where size matters
  -   Solid tumor indications

 

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Commercial Synergies

 

Key Products

    Hematology
    Solid Tumors

TRISENOX®

   

APL, CML, MDS,

Multiple myeloma

     

Pixantrone

   

Aggressive NHL

Indolent NHL

   

Breast cancer

Prostate cancer

XYOTAX

        

NSC lung cancer

Ovarian cancer

CT-2106

        

Colorectal cancer

Small cell lung cancer

 

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Hematology

Commercial opportunity

 

     2002 Incidence
    2002 Prevalence

Total Hematologic

    94,850    423,564

TRISENOX®

          

APL

    1,050    2,535

Myelodysplastic

          

Syndromes

    15,200    35,562

Multiple Myeloma

    14,600    49,542

Pixantrone

          

AML

    10,600    18,980

Indolent NHL

    24,030    142,625

Aggressive NHL

    29,370    174,320

 

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Selected Companies

Focused on Hematology Market

 

Company

   

Key Products

    Market Cap

Genentech

    Rituxan®    $ 38 B

Berlex*

    Campath®, Fludara®, Leukine®    $ 10 B

Idec

    Zevalin®, Rituxan®    $ 6.3 B

Millennium

    Velcade    $ 4.7 B

Celgene

    Thalomid®, Revimid    $ 2.7 B

CTI

    TRISENOX®, Pixantrone    $ 518 M1

 

*   Schering AG
1   Pro forma market cap

 

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Hematology Market Dynamics

 

  Few “big pharma” competitors in the space
  High incidence diseases with few good treatment options
  Concentrated target market
  -   ~4,500 physicians allows maximum sales and marketing leverage
  Many agents used in combination therapy

 

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Oncology

Commercial opportunity

 

     2002 Incidence
    2002 Prevalence

Total Oncologic

    516,144    3,132,334

XYOTAX

          

Advanced NSC lung

    137,600    162,352

Ovarian

    25,400    145,831

CT-2106

          

Small cell lung

    34,380    57,983

Colorectal

    147,500    930,083

Pixantrone

          

Breast

    212,600    1,836,085

 

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Companies Focused on

Oncology-Chemotherapy Market

 

Company

   

Key Products

    Market Cap

Pfizer

    Camptosar®    $ 285 B

GlaxoSmithKline

    Hycamtin®, Navelbine®    $ 126 B
             

Novartis

    Femara, Aredia®, Gleevec,    $ 117 B
     Sandostatin®, Zometa       
             

Astra-Zeneca

    Arimidex®, Casodex®, Faslodex®,    $ 78 B
     IRESSA®, Nolvadex®, Zoladex®       

Eli Lilly

    Gemzar®    $ 78 B

Bristol Myers

    Taxol®, Ifex®, Paraplatin®    $ 56 B

Aventis

    Taxotere®, Campto®, Genasense    $ 42 B

CTI

    XTOTAX, Pixantrone    $ 518 M1

 

1   Pro forma market cap

 

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Oncology Market Dynamics

 

  “Big pharma” significant sales and marketing presence provides barrier to new marketer entry
  Novel breakthrough products rapidly adopted and can generate >$1B in annual sales
  Suggests partnership with multi-nationals for blockbuster product may maximize commercial potential

 

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Commercial Strategy

 

  Utilize TRISENOX® to establish a commercial organization
  Expand TRISENOX® indications to capture market share in blood related cancers (MDS, multiple myeloma) making commercial business profitable
  Acquire additional products with utility in blood related cancers to expand market share and revenue growth
  Grow commercial organization to provide demand generating capacity for launch of XYOTAX

 

25

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CTI-Novuspharma Merger

Immediate realizable synergies

 

  Pixantrone: commercially attractive phase III product
-   May qualify for FDA fast track
-   Potential NDA 2005, market launch 2006
-   US sales could reach $150M+

 

  Financially attractive
-   $120M in cash
-   $18-$20M in cost savings
  Significant operating synergies
-   Critical mass in “global” oncology drug development
-   Increases commercial capabilities and sales potential in EU for expanded TRISENOX® label

 

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Strong Financial Position

 

  Pro-forma end Q1 cash position $306 million
-   $111M cash Q1-2003
-   $120M Novuspharma cash Q1-2003
-   $75M convertible offering*
-   Exchange offer 12/02 retired $60M convertible debt
  Merger offers potential for cost synergies
-   $18M to $20M savings in 2004
  TRISENOX® U.S. business becoming profitable
-   Allows ability to grow TRISENOX® sales in EU with new indication (MDS)
  Creates critical mass in cancer drug development and commercialization

 

*   Gross proceeds

 

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Commercial Operations

Edward F. Kenney

Executive Vice President

Chief Operating Officer

[GRAPHIC]

 

We’re fighting cancer

 

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Trisenox

(arsenic trioxide) injection

 

Indicated for the induction or remission and

consolidation for patients with relapsed or

refractory acute promyelocytic leukemia (APL)

 

[GRAPHIC]

 

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TRISENOX®

 

  Product approved US and EU
  100% CAGR forecasted through 2003
  $150+ million peak US sales potential
  Gaining US market share
  EU penetration limited to initial label (APL)
  Potential for MDS filing in 2004 allows for re-evaluation of EU commercial potential and strategy

 

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TRISENOX

US Patient Mix

 

1Q02

  

1Q03

APL 15%

  

APL 10%

Myeloma 43%

  

Myeloma 43%

MDS 29%

  

MDS 41%

Other 13%

  

Other 6%

 

[Graphic]

 

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TRISENOX®

Sales revenues & forecasts

$Millions

               

$6.0M

    $11.7M    $24M    $43.0M

2001

    2002    2003(E)    2004(E)

Source for 2004 estimate: CIBC World Markets

 

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Solid Tumors

Commercial opportunity

 

Taxanes

-   Taxol® (paclitaxel), Taxotere® (docetaxel) most widely used cancer drugs
  Worldwide sales exceed $2 billion
  Projected number of patients treated monthly
-   Paclitaxel – 54,700
-   Docetaxel – 26,400
  70% of taxane use is in 4 tumor types

 

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Worldwide Taxane Sales

2002

 

Paclitaxel $857M Sales 60% in ovarian and lung cancers

Docetaxel $1,192M WW Sales 33% in ovarian and lung cancers

 

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US Taxane Sales

2001

 

¨ Paclitaxel        ¨Docetaxel

NSC Lung Cancer    36,526 pts/yr. (Docetaxel) $153M     50,134 pts/yr (Paclitaxel) $280M

Ovarian Cancer     18,002 pts/yr (Paclitaxel) $195M

Breast Cancer     17,837 pts/yr (Docetaxel) $244M     15,923 pts/yr (Paclitaxel) $173M

 

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XYOTAX (polyglutamate paclitaxel)

 

A safer, potentially more effective taxane

 

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XYOTAX

Target product profile

     XYOTAX
    Paclitaxel
    Docetaxel

Premedications

    No    Yes    Yes

Infusion time

    10 mins    3 hrs    1 hr

Special infusion kits

    No    Yes    Yes

Hair loss

    No    Yes    Yes

Neuropathy

    Infrequent    Frequent    Infrequent

Tolerability

    Excellent    Fair    Fair

Efficacy

    Superior    —      —  

 

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Value Drivers

 

Drivers of market share

  Strength of product attributes
-   Efficacy
-   Safety
-   Convenience
  Reimbursement/third-party provider support
  Price/dosing schedule for XYOTAX

 

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Commercial Growth

[GRAPHIC]

 

TRISENOX® APL label, > 40 trials, 2003

 

XYOTAX Phase III trials, 2003

 

TRISENOX® Potential MDS label, 2004

 

XYOTAX

Potential NDA, 2004

 

Pixantrone

Phase III trials, 2004

 

TRISENOX® Potential myeloma label, 2005

 

XYOTAX

Potential NSCLC label, 2005

 

Pixantrone

Potential NDA, 2005

 

Pixantrone Potential aggressive NHL label, 2006

 

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Research & Clinical Development

Jack W. Singer

Executive Vice President

Research Chair

[GRAPHIC]

 

We’re fighting cancer

 

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Oncology Pipeline

 

    Preclinical    Phase I    Phase II    Phase III    NDA    Marketed

TRISENOX®

  

Approved for relapsed or refractory acute promyelocytic leukemia (APL)

Multiple myeloma, myelodysplasia, myelogenous leukemia and other cancers

XYOTAX

  

Non-small cell lung and ovarian cancers

Pixantrone

  

Non-Hodgkin’s lymphoma

CT-2106

  

Advanced solid tumors

LPAAT-B

    

inhibitors

    

 

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TRISENOX®

 

  Initial label indication: relapsed/refractory APL
  Compelling efficacy in other hematologic cancers (multiple myeloma, MDS)
  Robust safety data base of over 2,300 patients
-   Manageable side effect profile
  >40 market expansion investigator sponsored trials targeting larger disease targets

 

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TRISENOX®

Impressive efficacy data in MDS

 

MDS (145 patients, 81 evaluable)

  32% objective responses including high risk patients
  Decreases or eliminates RBC and platelet transfusion dependence
-   80% of responding pts became transfusion independent lasting up to 2 yrs
  Well tolerated, no dose reductions required
  Exploring label expansion in MDS in US and EU in 2004

Reported at conferences in May, 2003

 

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TRISENOX®

Impressive efficacy data in multiple myeloma

 

Multiple myeloma (86 patients, 78 evaluable)

  High response rates in combination with dexamethasone, vitamin C, and melphalan
-   ~40% objective responses (³ PR)
-   ~70% disease control
-   Marked improvement in kidney function
  Well tolerated; manageable side effects
  Active in patients who failed Velcade, Thalomid®
  2 large combination studies in progress
  Potential for label expansion

Reported at conferences in May, 2003

 

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XYOTAX

Safer, potentially more effective taxane

 

  Links paclitaxel to a “digestible” polymer
  Accumulates preferentially in tumor tissue
  Allows entry into cancer cells unlike standard paclitaxel
  10-minute infusion into peripheral vein; no premedications required
  Robust clinical development program
-   FDA approved phase III protocols for NSCLC
-   Several phase I/II clinical trials ongoing

 

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XYOTAX

Phase I/II clinical trials

 

  7 phase I trials
-   Single agent
-   Combined with platinates
-   Every other week dosing
-   Combined with radiation
  4 phase II trials
-   High risk NSC lung cancer
-   Chemotherapy resistant colorectal cancer
-   Chemotherapy resistant ovarian cancer
-   Relapsed/refractory breast cancer

 

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XYOTAX

Registration strategy & timeline

 

  XYOTAX pivotal clinical trials to demonstrate
-   Superior survival compared to marketed taxanes in treatment of NSC lung cancer
-   Ease of use
-   Lower overall treatment costs
-   Lower incidence of severe side effects compared to approved agents
  Submit NSC lung cancer NDA in 2H04
  Follow-on data in front-line ovarian cancer to supplement market launch

 

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Pixantrone

(from Novuspharma merger)

  New DNA intercalator with improved efficacy and safety
  Now in phase III for NHL

 

[GRAPHIC]  

 

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DNA Intercalators

 

  Established efficacy
-   Cornerstone of chemotherapy for breast cancer, leukemias, and lymphomas
-   Standard treatment in blood-born tumors – curative
-   Breast cancer – highly effective as adjuvant and frontline therapy
-   Only therapy for advanced forms of multiple sclerosis
  However – problems with cardiotoxicity
-   Irreversible damage to heart muscle
-   Maximum cumulative dose in patient’s lifetime
-   Prevents use as repeat therapy

 

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DNA Intercalators

with improved efficacy and safety

 

  Novuspharma’s approach
-   Alter chemical groups responsible for free-radical production and cardiac toxicity

 

[GRAPHIC]

 

  Target markets
-   Unmet clinical need in second-line therapy (NHL)
-   Replace current DNA intercalators as safer treatment in first-line

 

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Pixantrone

 

     Doxorubicin
    Mitoxantrone
    Pixantrone

Efficacy in

    +++    ++    ++++

hematology

               

Efficacy in

    ++/+++    ++    ++

solid tumors

               

Safety

    +    ++    ++++

(esp. cardiac)

               

 

  Superior anti-tumor activity in P388 and L1210 murine leukemias vs. Dx and Mitox
  Curative in YC-8 murine lymphoma
  Wide therapeutic window—effective from 1/3 of MTD
  Synergism with Cisplatin and Rituxan

 

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Effect of pixantrone and mitoxantrone (MITOX) on survival in the YC-8 lymphoma model (iv/iv + 1,5,9)

 

[Graphic]

 

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Pixantrone Experimental cardiotoxicity

 

[Graphic]

 

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Pixantrone

Target product profile

 

  Superior safety
-   Cardiac toxicity profile superior to existing agents
-   Not toxic to tissues, eliminates need for central line
-   Less severe nausea and vomiting
  Impressive efficacy
-   Long lasting complete remissions in heavily treated NHL patients
-   As single agent or in combination with chemotherapy
  Potential to be used where other anthracyclines cannot
-   Breast cancer in combination with Herceptin®
-   Breast cancer salvage after prior anthracycline therapy
-   Late-stage lymphomas

 

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Pixantrone

 

  Extensive clinical trial experience
-   >170 patients
-   7 phase I, II trials
  Initial market entry into area of high unmet need
-   3rd-line aggressive NHL
-   Currently no approved therapies
-   Market size ~15,000 patients
  Potential label expansion
-   Relapsed indolent NHL + Rituxan® (phase III)
-   2nd-line combination in high grade NHL (phase II)
-   Salvage breast cancer ± Herceptin® (planned)

 

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Pixantrone

Impressive single agent activity (NHL)

 

  High response rates in relapsed/resistant aggressive NHL
-   ORR= >30% (7CRs/5PRs + 5uPRs)
-   Durable responses: TTP >8 months for responders
  Well tolerated
-   Grade 4 neutropenia 13/33 (40%)
-   Grade 4 anemia/thrombocytopenia 0-1/33 (<3%)
  28/33 (85%) had maximum prior anthracycline exposure
  14/33 (42%) received >1,000-1500mg/m2 Pixantrone
  Encouraging low incidence of cardiac events despite prior anthracycline exposure

 

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Pixantrone

Combination trials

 

  Highly active in combination regimens for relapsed/refractory NHL replacing doxorubicin
-   CHOP n=17
  13 patients evaluable; 6CRs/1PR
-   ESHAP n=21
  19 patients evaluable; 7CRs/4PRs
  Highly active in relapsed/refractory indolent NHL
-   FND-R n=9
-   6 patients evaluable; 5CRs/1PR

 

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Preliminary Market Study

% of physicians who would prescribe Pixantrone

by line of therapy

 

     First Line
     Second Line
     Third Line
  

Aggressive

    47 %   100 %   100 %

Indolent

    27 %   67 %   67 %

 

-   Almost half of the physicians would try Pixantrone in place of doxorubicin in first line therapy for aggressive patients – mostly for patients with cardiovascular risk factors

 

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CT-2106

Polyglutamate camptothecin

 

  Camptothecins (irinotecan, topotecan) approved for colorectal cancer, small cell lung cancer, and relapsed ovarian cancer
  Highly active class of drugs but limited by toxicity
  CT-2106 links 20S camptothecin to PG polymer
  Excellent activity and safety in animal studies
  Preliminary phase I data
-   13 patients treated at doses from 12 to 75 mg/m2
-   MTD not reached
-   Early evidence of activity
-   Presentation on preliminary results targeted for 4Q03
  Plan to initiate phase I/II combination study in colorectal and/or small cell cancer in 1H04

 

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LPAAT-ß

Novel cancer target

 

  LPAAT-ß cloned and identified as a novel cancer target by CTI scientists
  Potential broad utility against many types of common cancers
  Preclinical studies of drug-like inhibitors selectively destroy cancerous cells
  Plenary presentations at three major cancer meetings in 2002 -2003
  Potential clinical candidate in 2004

 

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Closing Remarks

James A. Bianco

President and CEO

We’re fighting cancer

[GRAPHIC]

 

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Last 12 Months in Review

Objective

  Acquire late stage or commercial product
  Reduce burn rate and secure adequate capital to grow commercial operations and see XYOTAX to NDA
  Advance discussions toward potential XYOTAX partner
  Initiate pivotal XYOTAX phase III trials
  TRISENOX®—profitable operating business
  Highlight clinical data at key scientific meetings

 

Status

  Novuspharma merger
-   Pixantrone in phase III
-   $18-$20m in annual operating synergies
-   $120M balance sheet
  $75M notes offering
  Partnership discussions for XYOTAX ongoing
  STELLAR-2, -3, -4 trials FDA approved and enrolling
  Sales targeted to double to $24M this year
  ASH, AACR, ASCO, MM, MDS

 

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Key Objectives

Next 12-18 Months

 

  Gynecologic Oncology Group to initiate phase III study of XYOTAX in ovarian cancer
  Complete enrollment of pivotal trials in non-small cell lung cancer
  Successful merger with Novuspharma to maximize cost synergies and efficiencies
  Initiate pivotal trial of Pixantrone in aggressive relapsed NHL

 

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Key Objectives

Next 12-18 Months

 

  Explore TRISENOX® label expansion in MDS in 2004
  Grow TRISENOX® sales >$40M
  Submit NDA for XYOTAX
  Advance LPAAT inhibitors in development
  Secure global commercial partner for XYOTAX

 

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Stock Price Performance

 

[Graphic]

 

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Community Involvement

 

International Myeloma Foundation    Education-Treatment-Research

The Leukemia & Lymphoma Society    Fighting Blood-Related Cancers

MMRF Multiple Myeloma Research Foundation

Gilda’s Club Worldwide

The Friends of José Carreras International Leukemia Foundation

Lance Armstrong Foundation

Ronald McDonald House - The House that love built. Seattle

Seattle Center Foundation

MS National Multiple Sclerosis Society

Fred Hutchinson Cancer Research Center

United Way of America

 

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[Graphic] cti

Making cancer more treatable

(c) 2003 Cell Therapeutics Inc

 

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