Pipeline/Commercial Insight: Innovative Targeted Therapies - 'Smart Drugs' on Target for Increasing Growth

Table of Contents

ABOUT DATAMONITOR HEALTHCARE

• About the Oncology pharmaceutical analysis team
  • Richard Faint - Director of Oncology

CHAPTER 1 EXECUTIVE SUMMARY

• Scope of analysis
• Datamonitor insight into the targeted therapies market

CHAPTER 2 PIPELINE OVERVIEW

• Pipeline overview
• Pipeline by developmental phase & class of drug
  • Signal transduction inhibitors and angiogenesis inhibitorsconstitute over half the current targeted therapies pipeline
    • Signal transduction inhibitors & angiogenesisinhibitors dominate due to their wide applicability for use and provensuccess in the market to date
    • Setbacks suffered by Gentas Genasense may have deterredother developers of apoptosis stimulators
    • The specificity of monoclonal antibody target meanspatient potential is restricted, however, success of Rituxan may spurdevelopers on
    • The HDAC inhibitors & cell cycle regulators arerestricted in terms of potential molecular target, hence their minimalpresence in the pipeline
  • The current late-phase pipeline is relatively sparse dueto the novelty of this market
    • As time progresses, the late-phase pipeline will flourishas early-phase candidates move forward in development
• Pipeline by molecular target
  • Signal transduction inhibitors
    • The EGFR and multiple tyrosine kinases remain the focus ofdevelopment as targets for signal transduction inhibitors
  • Angiogenesis inhibitors
    • The VEGFR and multiple tyrosine kinases remain the focusof development as targets for angiogenesis inhibitors
  • Apoptosis stimulators
    • Due to a lack of information from developers, a populartarget for apoptosis is difficult to identify
  • HDAC inhibitors
  • Cell cycle regulators
    • Utility of CDK as a target comes from known mutation/overexpressionin some malignancies
  • Other monoclonal antibodies
    • The CD family of proteins allows for a highly specifictarget, with proven success via Rituxan
• Pipeline by indication
  • The big four tumor types, plus melanoma and RCC are themost popular indications for development
    • Constituting over half of all newly diagnosed cancercases, the big four tumor types offer significant commercial potential
    • Melanoma and RCC are well characterized in terms of tumorgrowth drivers, thus making them ideal indications for the development oftargeted therapies
  • Non-Hodgkins lymphoma dominates the pipeline within thehematological malignancies
    • Based on incidence rates, non-Hodgkins lymphoma is themost commercially attractive hematological indication for development
    • Pipeline compounds for leukemia are similar across thedifferent types, due to potential for horizontal expansion
• Pipeline by company
  • At least 138 companies are involved in the currenttargeted therapies pipeline
    • The majority of pipeline compounds are in early-phasetrials, hence two-thirds of companies involved are small biotechnologyfirms
  • Top three companies in terms of marketed and pipelineproducts are Genentech, AstraZeneca and Pfizer
    • Genentech
    • AstraZeneca
    • Pfizer
• Key metrics
• Datamonitor pipeline assessment summary

CHAPTER 3 PIPELINE DYNAMICS

• A diverse range of disease subtypes
• Genetic basis of cancer evolution
  • Tumorigenesis is the result of cooperative accumulatedmutations
• Existing pharmacotherapy approaches provide limitedtreatment benefit
  • Cytotoxic drugs lack specificity
  • Hormonal or endocrine therapy provides incremental benefitin selected tumors
  • Optimizing current treatment strategies is paramount
• The emergence of targeted treatment heralds a revolutionin cancer pharmacotherapy
• Dynamic cancer market offers significant commercialopportunity
  • Ongoing sales growth drives the market
  • Intensive R&D produces a rich developmental pipeline
  • Growing patient population and significant unmet needspropel innovation in the cancer market
    • Cancer epidemiology - an expanding patient base
    • Significant areas of unmet need persist
• Clinical and strategic threats to the commercialization ofcancer drugs
  • Progressively rising R&D costs threaten industryproductivity
    • High attrition rates can be mitigated by improvedstrategic decision-making
    • Lengthening drug approval process a consequence ofincreased regulatory demands
  • Pharmacoeconomic pressures drive payers to implementrestrictive pricing and reimbursement policies
  • Increased therapeutic and generic competition results inreduced periods of market exclusivity
  • Segmentation of market will require changes in clinicaltrial methodology

CHAPTER 4 MARKET DEFINITION & PIPELINE CLASSIFICATION

• Targeted therapies overview
  • The development of innovative targeted therapies
    • Current therapies adversely affect non-malignant cells
    • Innovative targeted therapies can address novel propertiesof tumor cells to selectively target them over normal cells
    • Key issue is the identification of targets unique tocancer cells
• Market definition
  • L1X3 - Antineoplastic monoclonal antibodies
  • L1X9 - All other antineoplastics
• Classification of pipeline products
  • Signal transduction inhibitors
    • A plethora of potential targets along the signalingcascade exist
    • Several signal transduction inhibitors have reached themarket, bringing with them their own sets of issues for consideration
  • Angiogenesis inhibitors
    • Angiogenesis as a normal biological process
    • Angiogenesis is known to be abberant in tumor cellproliferation
    • Angiogenesis inhibitors as viable antitumor agents cantarget a number of pathways
    • At present, only one angiogenesis inhibitor exists in themarket
  • Apoptosis stimulators
    • Cell death can be induced via a number of differentpathways
    • To date, only one apoptosis stimulator has reached themarket
  • Histone deacetylase inhibitors
    • Despite relative immaturity of development in this classof drugs, the potential to enhance current therapies exists
  • Cell cycle inhibitors
    • Despite ongoing R&D efforts, all current candidatesremain in the Phase II stage of development
• Pipeline comparator
• Current market situation

CHAPTER 5 MARKETED PRODUCTS FORECAST ANALYSIS

• Country-specific assumptions and effects
  • Effect of Medicare Modernization Act in the US
  • Biennial price cuts in Japan
  • National Institute of Clinical Excellence in the UK
• Product assumptions and effects
  • Signal transduction inhibitors
    • Erbitux (cetuximab)
    • Gleevec (imatinib)
    • Herceptin (trastuzumab)
    • Iressa (gefitinib)
    • Tarceva (erlotinib)
    • Targretin (bexarotene)
  • Angiogenesis inhibitors
    • Avastin (bevacizumab)
  • Apoptosis stimulators
    • Velcade (bortezomib)
  • Other monoclonal antibodies
    • Bexxar (tositumomab)
    • Campath (alemtuzumab)
    • Mylotarg (gemtuzumab)
    • MabThera/Rituxan (rituximab)
    • Zevalin (ibritumomab)
  • Others
    • Ontak (denileukin)
• Forecasts

CHAPTER 6 PIPELINE SIGNAL TRANSDUCTION INHIBITORS ANALYSIS& FORECASTS

• Pipeline overview
• Onyx Pharmaceuticals/Bayers sorafenib (BAY 43-9006)
  • Drug profile
    • Multi-targeted approach allows for clinical development ina wide range of tumors
  • Clinical trial data
    • Sorafenib in RCC moves into preregistration
    • Potential for monotherapy and combination therapy in HCC
    • Combination therapy provides opportunity in malignantmelanoma
    • Phase II clinical trials
    • Acceptable toxicity profile
  • Datamonitor comments
    • Despite sorafenibs convincing single-agent activity, fullpotential will lie in combination regimens
    • Potential first-to-market status and collaboration willensure sorafenib is the leading multi-kinase inhibitor
• Pfizers Sutent (sunitinib malate)
  • Drug profile
    • Development is ongoing in a variety of tumors due to wideapplicability of use of Sutent
  • Clinical trial data
    • Sutent shows significant activity among refractory GISTpatients with no alternative treatment options
    • Significant activity shown in second-line treatment ofRCC, though ongoing Phase III study is exploring first-line Sutentmonotherapy
    • Ongoing Phase II trial in breast cancer followingencouraging preliminary results
    • Activity shown in difficult to treat population withneuroendocrine tumors, although large-scale trials are yet to be initiated
    • Phase II clinical trials
    • Majority of Sutents toxicities are mild in nature
  • Datamonitor comments
    • Initial regulatory approval will come via GIST patients,although product expansion will need to occur to increase commercialpotential
    • Pfizers presence will be advantageous once Sutent gainsmarketing approval
• Abbott Laboratories Xinlay (atrasentan)
  • Drug profile
    • Xinlays target receptor plays a key role in cancer cellproliferation
  • Clinical trial data
    • ODAC decision indicates low probability of Xinlay beinggranted FDA approval for prostate cancer
    • Activity of Xinlay in NSCLC similar to standardchemotherapy
    • Other trials
  • Datamonitor comments
    • Clinical benefit among a patient population with fewtreatment options means Xinlay could fulfill a significant unmet need
    • Abbotts favorable position in the prostate cancer marketwill be invaluable in Xinlays market potential
• Abgenix/Amgens ABX-EGF (panitumumab)
  • Drug profile
    • Overexpression of EGFR makes an ideal target for ABX-EGFdevelopment
  • Clinical trial data
    • ABX-EGF shows promise as monotherapy or combinationtherapy across a range of treatment settings for colorectal cancer
    • Addition of ABX-EGF appears to enhance standardchemotherapy in NSCLC
    • Poor results as a single agent in RCC
    • Termination of development in prostate cancer
    • Main side effect is a potential indicator of ABX-EGFactivity
  • Datamonitor comments
    • Humanized nature of ABX-EGF holds some advantages overcompetitor EGFR inhibitors
    • Way forward for Amgen lies in ABX-EGF combination regimensand potential development of biomarker
    • Amgens presence will ensure success, althoughprofitability may increase by targeting earlier lines of therapy
• GlaxoSmithKlines lapatinib (GW-572016)
  • Drug profile
    • Lapatinib is unique among the EGFR inhibitors by targetingtwo receptor tyrosine kinases
  • Clinical trial data
    • HER-2 overexpression in breast cancer justifies validityof lapatinibs target
    • Limited single-agent activity indicates combinationregimens including lapatinib are the way forward in NSCLC
    • Limited activity has terminated development of lapatinibin colorectal cancer
    • Modest activity in urothelial tumors, although unclearwhether GlaxoSmithKline intends to pursue this indication
    • Infrequent incidence of Grade 3 or higher toxicity
  • Datamonitor comments
    • Initial approval in niche breast cancer indication willexpedite subsequent approvals, with potential blockbuster status forlapatinib
    • GlaxoSmithKline needs to account for deficiency inoncology market experience to take full advantage of lapatinibs potential
• Schering-Ploughs Sarasar (lonafarnib)
  • Drug profile
    • Previously wide range of developmental indications forSarasar has been reduced to just two
  • Clinical trial data
    • Main focus of Sarasar development in MDS, where greatestantitumor activity is shown
    • Lack of efficacy has led to termination of pivotal PhaseIII trial in NSCLC
    • Lack of clinical data makes it difficult to judgeSarasars potential in breast cancer
    • Benefit shown in advanced head and neck cancer, althoughno further trials have been announced
    • Limited activity as a single agent, although Sarasar mayshow potential in combination therapy in pancreatic cancer
    • Despite encouraging Phase II results in urothelial tractcarcinoma, no further clinical trials are planned
    • Lack of single-agent activity in colorectal cancer hashalted development in this indication
    • Mild toxicity in the majority of patients, although Grade3 events do occur
  • Datamonitor comments
    • The FDAs recent rejection of Johnson & JohnsonsZarnestra may reduce the time between launches of the two farnesyltransferase inhibitors
    • Presence in oncology market will aid commercialization ofSarasar
• Wyeths temsirolimus (CCI-779)
  • Drug profile
    • Temsirolimus inhibits a key pathway in tumor cellproliferation
  • Clinical trial data
    • Encouraging response rates seen for temsirolimus incombination with standard interferon-alfa for RCC in Phase I trials arebeing further investigated
    • Substantial antitumor activity in Phase II trials inmantle cell lymphoma led to initiation of a Phase III trial in January2005
    • Temsirolimus shows activity as a single agent and incombination with hormonal therapy in breast cancer
    • Temsirolimus shows some activity in SCLC, although Wyethhas not stated its intention to pursue this indication
    • Temsirolimus does not show activity as a single agent inmelanoma
    • Despite encouraging results, Wyeth is not pursuingglioblastome multiforme as a potential indication for temsirolimus
    • Mild toxicity means temsirolimus is well tolerated
  • Datamonitor comments
    • Lucrative opportunites exist for temsirolimus, althoughbroad commercialization would be expedited via an approval in a nicheindication
    • Prior commercialization of Mylotarg has given Wyeth theexperience to launch temsirolimus successfully
• AstraZenecas Zactima (ZD-6474)
  • Drug profile
    • Zactimas ability to inhibit both angiogenesis and signaltransduction should in theory result in greater efficacy in certainpatient subsets
  • Clinical trial data
    • Phase III trials investigating Zactima in NSCLC areplanned for second half of 2005
    • Phase II trial in multiple myeloma failed to meet primaryendpoint
    • Other trials
  • Datamonitor comments
    • Zactimas survival benefit in NSCLC needs to be convincingin order to compete with Tarceva
    • AstraZenecas strength in the oncology market will be keyin Zactimas success
• Janssen/Johnson & Johnsons Zarnestra (tipifarnib)
  • Drug profile
    • Previously wide range of developmental indications forZarnestra have been reduced to just one
  • Clinical trial data
    • Following rejection of an NDA, the FDA requires Phase IIIdata for Zarnestra in AML before regulatory approval can be considered
    • Zarnestra shows activity in MDS, although further study isnot planned in short-term future
    • Negative Phase III trial results caused termination ofdevelopment in pancreatic cancer
    • Negative Phase III trial results caused termination ofdevelopment in colorectal cancer
    • Zarnestra development in breast cancer remains in Phase IItrials
    • Minimal activity in prostate cancer has terminateddevelopment in this indication
    • Lack of activity in SCLC caused termination of Phase IItrial
    • Phase I trial is ongoing for Zarnestra in combination withchemotherapy in advanced NSCLC
    • Despite modest activity in brain cancer, follow-up trialshave not been initiated
    • Mild toxicity is particularly significant sinceZarnestras main indication is for elderly AML patients where quality oflife is a major issue
  • Datamonitor comments
    • FDA rejection has caused Zarnestra to lose its lead
    • Focus on gene expression profiling may lead tofragmentation of the market
    • Johnson & Johnsons experience will be invaluable toZarnestra
    • Zarnestras niche indication may dilute effects of itsprobable first-to-market status loss
• Bristol-Myers Squibbs dasatinib (BMS-354825)
  • Drug profile
    • Dasatinib shows potential to overcome Gleevec resistance
  • Clinical trial data
    • Dasatinib overcomes Gleevec resistance in CML patients
    • Phase I study of dasatinib in solid tumors is ongoing
  • Datamonitor comments
    • Despite convincing clinical benefit, dasatinib alreadyfaces potential competition from Novartiss AMN-107
    • Bristol-Myers Squibbs extensive oncology experience willaid commercializatioan of dasatinib
• Novartiss AMN-107
  • Drug profile
    • AMN-107 shows potential for greater efficacy than Gleevec
  • Clinical trial data
    • AMN-107 confers significant activity in Gleevec-resistantCML
  • Datamonitor comments
    • AMN-107 in a race with Bristol-Myers Squibbs dasatinib toreach the market first
    • An opportunity for Novartis to consolidate and expand itsleading role in the CML therapy market
• Kosan Biosciences 17-AAG
  • Drug profile
    • Potential to disrupt a host of relevant oncology targetsmeans 17-AAG shows a wide range of applicability
  • Clinical trial data
    • 17-AAG as a single agent induced disease stabilization inmelanoma patients
    • 17-AAG with docetaxel resulted in minor tumor responses
    • 17-AAG with gemcitabine and cisplatin resulted in twopartial responses
    • Some evidence of 17-AAG activity in multiple myeloma
    • Phase II trials
  • Datamonitor comments
    • Although 17-AAGs formulation may provide setbacks,commercial potential can be increased by developing biomarkers to judgeresponse
    • Kosan Biosciences should recruit the experience andresources of a key oncology player
• Forecasts
• Datamonitor drug assessment summary

CHAPTER 7 PIPELINE ANGIOGENESIS INHIBITORS ANALYSIS &FORECASTS

• Pipeline overview
• National Cancer Institutes CAI (L-651582,carboxyamidotriazole)
  • Drug profile
    • Clinical trials completed in a range of tumor types,although further development is unclear
  • Clinical trial data
    • Phase III trial failed to demonstrate any benefit of CAIover placebo in NSCLC
    • Limited evidence for future development of CAI in RCC
    • Some activity in ovarian cancer, although furtherdevelopment is unclear
  • Datamonitor comments
    • CAI left virtually redundant by Avastin and otherlate-stage pipeline angiogenesis inhibitors with superior clinicalprofiles
    • Success of CAI depends solely on involvement of apharmaceutical company, which is unlikely to occur
• Aterna Zentariss Neovastat (AE-941)
  • Drug profile
    • Development of Neovastat scaled down to focus solely onNSCLC
  • Clinical trial data
    • Final results from Phase III trial in NSCLC expected in2006
    • Termination of Neovastat development in RCC followingfailure of Phase III to meet its primary endpoints
    • Other indications
  • Datamonitor comments
    • If ongoing Phase III trial does not meet its primaryendpoints, it could be the end for development of Neovastat
    • Aterna Zentaris should secure a US marketing partner inorder to increase commercial potential of Neovastat
• Novartis/Schering AGs PTK-787 (vatalinib)
  • Drug profile
    • By targeting all known VEGFR tyrosine kinases, PTK-787should show activity across a range of tumor types
  • Clinical trial data
    • Anticipated regulatory filing for PTK-787 in colorectalcancer delayed to 2007 following disappointing CONFIRM-1 interim results
    • Recent initiation of the Phase II GOAL Study in NSCLC
    • Phase II trial is ongoing for PTK-787 in glioblastomamultiforme
    • Development in other tumors remains in early phases
    • Majority of reported toxicities among 1,000 patients havebeen mild to moderate in nature
  • Datamonitor comments
    • PTK-787s distinct advantages could recoup any negativerepurcussions from the CONFIRM-1 interim results
    • Schering AG and particularly Novartiss prior oncologyexperience will be invaluable to PTK-787
• Pfizers AG-13736
  • Drug profile
  • Clinical trial data
    • AG-13736 shows substantial antitumor activity incytokine-refractory metastatic RCC
    • AG-13736 does not confer significant activity as a singleagent in AML and MDS
    • Demonstration of AG-13736 activity in Phase I study insolid tumors forms the basis of ongoing Phase II trials
  • Datamonitor comments
    • With a strategic development plan, Pfizer may be able toovercome Avastins leading position
    • Pfizers experience will be advantageous in thedevelopment of AG-13736
• Forecasts
• Datamonitor drug assessment summary

CHAPTER 8 PIPELINE APOPTOSIS STIMULATORS ANALYSIS &FORECASTS

• Pipeline overview
• Gentas Genasense (oblimersen)
  • Drug profile
    • Despite termination of Gentas agreement withSanofi-Aventis, Genasense remains in development for a multitude ofindications
  • Clinical trial data
    • Benefits of Genasense in CLL may not be enough to offsetthe addition of significant toxicity
    • Long-term survival results of Genasense in malignantmelanoma are of significance
    • Disappointing Phase III trial results in multiple myelomameans status of further development is unclear
    • Early-phase benefits of Genasense in AML requireconfirmation in Phase III clinical trial
    • Lack of clinical data in NSCLC makes it difficult to judgeGenasenses potential
    • Encouraging Phase II results in prostate cancer, thoughPhase III trials have yet to be initiated
    • Ongoing Phase II trial in SCLC will determine if patientbenefit counters additional toxicity
    • Promise shown in combination with rituximab in NHL, butrandomized trials have yet to be initiated
    • Genasense did not enhance activity of standardinterferon-alfa in RCC
    • Other trials
  • Datamonitor comments
    • Wide range of developmental indications for Genasenseprovides Genta with a significant commercial opportunity
    • Termination of agreement with Sanofi-Aventis is a majorsetback for Genta
• Teliks Telcyta (TLK286)
  • Drug profile
    • Synergy of Telcyta with standard cytotoxics may indicate awide ranging applicability for use
  • Clinical trial data
    • Convincing Phase II results have initiated two large-scalePhase III trials in ovarian cancer
    • Benefit of Telcyta in combination with standardchemotherapy shown in NSCLC
    • Telcyta shows some activity as a single agent in breastcancer, although final Phase II results have yet to be published
    • Uncertain status of Telcyta in colorectal cancer
  • Datamonitor comments
    • Telik should seek initial approval of Telcyta in ovariancancer, which should expedite subsequent submissions
    • In light of the competition Tarceva will provide forTelcyta, Telik would be prudent in seeking a commercialization partner
• Xenovas TransMID (XR-311)
  • Drug profile
    • TransMIDs target is highly relevant in brain cancer
  • Clinical trial data
    • Encouraging Phase II results, active clinical trialprogram and fast-track designation will drive development of TransMID
  • Datamonitor comments
    • Cumbersome infusion schedule and administration maydetract from TransMIDs broad clinical benefit
    • Although Xenova has secured several marketingpartnerships, a glaring omission is one in the lucrative US market
• Forecasts
• Datamonitor drug assessment summary

CHAPTER 9 PIPELINE HISTONE DEACETYLASE INHIBITORS ANALYSIS& FORECASTS

• Pipeline overview
• Gloucester Pharmaceuticals FK-228 (depsipeptide)
  • Drug profile
    • Broad range of HDAC inhibition should theoreticallyprovide increased efficacy
  • Clinical trial data
    • Encouraging results in cutaneous T-cell lymphoma requirereplication in ongoing Phase III clinical trial
    • A lack of clinical data exists, despite FK-228s Phase IIstatus in prostate cancer and RCC
  • Datamonitor comments
    • FK-228 likely to become the first HDAC inhibitor to reachthe market
    • Commercial success of FK-228 will rely on GloucesterPharmaceuticals collaborating with large pharma
• Forecasts
• Datamonitor drug assessment summary

CHAPTER 10 OTHER PIPELINE MONOCLONAL ANTIBODIES ANALYSIS& FORECASTS

• Pipeline overview
• Millennium Pharmaceuticals/BZL Biologicss MLN-2704
  • Drug profile
    • MLN-2704 has been developed specifically for prostatecancer
  • Clinical trial data
    • High doses of MLN-2704 resulted in tumor response andreduction in PSA levels in progressive, metastatic HRPC patients
  • Datamonitor comments
    • Significant opportunity lies in the prostate cancermarket, although future expansion could occur within other tumor types
    • Experience gained in commercialization of Velcade will beinvaluable in the development of MLN-2704
• Forecasts
• Datamonitor drug assessment summary

CHAPTER 11 COMMERCIAL IMPACT & LIFECYCLE MANAGEMENT:CASE STUDIES

• Introduction
• Case study 1
  • Iressa and Tarceva: why the difference?
    • How have two nearly identical drugs realized such varyinglevels of success in the NSCLC market?
    • Iressas Phase II survival benefit was sufficient togarner FDA approval
    • Concerns over Iressas potential toxicity restricted itsuse in Japan
    • FDA approval of Tarceva was based on a Phase III trialthat demonstrated a two-month survival benefit in the third-line NSCLCsetting
    • Phase III ISEL trial comparing Iressa with placebo inadvanced NSCLC failed to show survival benefit
    • Negative repercussions of the Iressas failed Phase IIItrial
    • Tarcevas potential is currently limited by Alimta in thesecond-line setting, although line extensions will increase uptake andsales
    • What if Iressa had not failed?
    • Could Iressa pose a threat to Tarceva?
    • Future opportunities are plentiful for Tarceva and Iressa
• Case study 2
  • Strategies for success: Genentech
    • A leading oncology player with winning strategies
    • Strengths and weaknesses of a collaborative partnership
    • The prime example
  • Strategies for success: Novartis
    • An entirely new strategy for the pharmaceutical industry
    • Early-phase development was slow...
    • ...although subsequent approval and launch was remarkablyquick
    • Approval for a second indication granted only nine monthsafter Gleevecs initial approval
    • Opportunities for continued growth exist...
    • ...although some drawbacks and threats have arisen
    • The rewards of this strategy are very attractive todevelopers
• Case study 3
  • The pharmacoeconomic challenges associated with targetedtherapies
    • Unique pharmacoeconomic challenges will arise as targetedtherapies are included in standard chemotherapy regimens
    • The cost of standard chemotherapy for cancer
    • The inclusion of targeted therapies into standardtreatment regimens
    • The impact of monoclonal antibody targeted therapies
    • The impact of small molecule targeted therapies
    • The problem of adding targeted therapies to standardchemotherapy regimens
    • Further effects of pharmacoeconomic issues
    • Communicating the value of targeted therapies

APPENDIX A - MARKET DATA & MAJOR BRAND KEY FACTS

• L1X3 (antineoplastic monoclonal antibodies) class marketdata
• L1X9 (all other neoplastics) class market data
• Sales data and forecasts
• PowerPoint Executive Presentation

• APPENDIX B - SALES FORECASTS
  • US forecasts
  • Japan forecasts
  • France forecasts
  • Germany forecasts
  • Italy forecasts
  • Spain forecasts
  • UK forecasts
  • EU5 forecasts
  • Global forecasts
• APPENDIX C
  • List of tables
  • List of figures
  • Methodology
    • Datamonitor forecast methodology
      • Forecasts for marketed drugs
      • Forecasts for pipeline drugs
    • Datamonitor drug assessment methodology
  • List of abbreviations
  • Contributing experts
    • US opinion leader 1
    • US opinion leader 2
  • Bibliography
  • About Datamonitor
    • About Datamonitor Healthcare
    • About the Oncology analysis team
• Disclaimer

List of Tables

• Table 1: Targeted therapies in preregistration, 2005
• Table 2: Targeted therapies in Phase III development,2005
• Table 3: Pipeline targeted therapies by developmentphase & class of drug, 2005
• Table 4: Pipeline signal transduction inhibitors bytarget, 2005
• Table 5: Pipeline angiogenesis inhibitors in developmentby target, 2005
• Table 6: Pipeline apoptosis stimulators in developmentby target, 2005
• Table 7: Pipeline cell cycle regulators in developmentby target, 2005
• Table 8: Pipeline monoclonal antibodies in developmentby target, 2005
• Table 9: Pipeline targeted therapies by indication, 2005
• Table 10: Genentechs marketed oncology portfolio, 2005
• Table 11: Genentechs pipeline oncology portfolio, 2005
• Table 12: AstraZenecas marketed oncology portfolio,2005
• Table 13: AstraZenecas pipeline oncology portfolio,2005
• Table 14: Pfizers marketed oncology portfolio, 2005
• Table 15: Pfizers pipeline oncology portfolio, 2005
• Table 16: Late-phase pipeline targeted therapies salesforecasts ($m), 2005-14
• Table 17: Datamonitor drug assessment summary
• Table 18: Common mutations involved in tumor development
• Table 19: Forecast incidence of cancer across the sevenmajor markets, 2005-13
• Table 20: Examples of naturally occurring angiogenesisstimulators
• Table 21: Current marketed products in the targetedtherapies market, (1 of 2)
• Table 22: Current marketed products in the targetedtherapies market, (2 of 2)
• Table 23: Targeted therapies sales in the seven majormarkets, 2003-04
• Table 24: Late-phase pipeline signal transductioninhibitors in development, 2005 (1 of 2)
• Table 25: Late-phase pipeline signal transductioninhibitors in development, 2005 (2 of 2)
• Table 26: Phase II pipeline signal transductioninhibitors in development, 2005 (1 of 2)
• Table 27: Phase II pipeline signal transductioninhibitors in development, 2005 (2 of 2)
• Table 28: Phase I pipeline signal transductioninhibitors in development, 2005
• Table 29: Ongoing clinical trials involving sorafenib
• Table 30: Ongoing clinical trials involving Sutent
• Table 31: Ongoing clinical trials involving Xinlay
• Table 32: Ongoing clinical trials involving ABX-EGF
• Table 33: Ongoing clinical trials involving lapatinib
• Table 34: Ongoing clinical trials involving Sarasar
• Table 35: Ongoing clinical trials involving temsirolimus
• Table 36: Ongoing clinical trials involving Zactima
• Table 37: Ongoing clinical trials involving Zarnestra
• Table 38: Ongoing clinical trials involving dasatinib
• Table 39: Ongoing clinical trials involving AMN-107
• Table 40: Ongoing clinical trials involving 17-AAG
• Table 41: Xinlay & Sutent forecasting assumptions
• Table 42: Sorafenib & ABX-EGF forecastingassumptions
• Table 43: Lapatinib & Sarasar forecastingassumptions
• Table 44: Temsirolimus & Zactima forecastingassumptions
• Table 45: Zarnestra, dasatinib & AMN-107 forecastingassumptions
• Table 46: Signal transduction inhibitors sales forecasts($m), 2005-14
• Table 47: Research/clinical and commercialattractiveness of pipeline signal transduction inhibitors (1 of 3)
• Table 48: Research/clinical and commercialattractiveness of pipeline signal transduction inhibitors (2 of 3)
• Table 49: Research/clinical and commercialattractiveness of pipeline signal transduction inhibitors (3 of 3)
• Table 50: Late-phase pipeline angiogenesis inhibitors indevelopment, 2005
• Table 51: Phase II pipeline angiogenesis inhibitors indevelopment, 2005
• Table 52: Phase I pipeline angiogenesis inhibitors indevelopment, 2005
• Table 53: Ongoing clinical trials involving Neovastat
• Table 54: Ongoing clinical trials involving PTK-787
• Table 55: Ongoing clinical trials involving AG-13736
• Table 56: PTK-787, Neovastat & AG-13736 forecastingassumptions
• Table 57: Angiogenesis inhibitors sales forecasts ($m),2005-14
• Table 58: Research/clinical and commercialattractiveness of pipeline angiogenesis inhibitors
• Table 59: Late-phase pipeline apoptosis stimulators indevelopment, 2005
• Table 60: Phase II pipeline apoptosis stimulators indevelopment, 2005 (1 of 2)
• Table 61: Phase II pipeline apoptosis stimulators indevelopment, 2005 (2 of 2)
• Table 62: Phase I pipeline apoptosis stimulators indevelopment, 2005
• Table 63: Ongoing clinical trials involving Genasense
• Table 64: Ongoing clinical trials involving Telcyta
• Table 65: Ongoing clinical trials involving TransMID
• Table 66: Genasense forecasting assumptions
• Table 67: Telcyta & TransMID forecasting assumptions
• Table 68: Apoptosis stimulators sales forecasts ($m),2005-14
• Table 69: Research/clinical and commercialattractiveness of pipeline apoptosis stimulators
• Table 70: Pipeline histone deacetylase inhibitors indevelopment, 2005
• Table 71: Ongoing clinical trials involving FK-228
• Table 72: FK-228 forecasting assumptions
• Table 73: FK-228 sales forecasts ($m), 2005-14
• Table 74: Research/clinical and commercialattractiveness of FK-228
• Table 75: Phase II/III pipeline monoclonal antibodies indevelopment, 2005 (1 of 2)
• Table 76: Phase II/III pipeline monoclonal antibodies indevelopment, 2005 (2 of 2)
• Table 77: Phase I pipeline monoclonal antibodies indevelopment, 2005
• Table 78: Ongoing clinical trials involving MLN-2704
• Table 79: MLN-2704 forecasting assumptions
• Table 80: MLN-2704 sales forecasts ($m), 2005-14
• Table 81: Research/clinical and commercialattractiveness of MLN-2704
• Table 82: Key Iressa & Tarceva events in the NSCLCmarket
• Table 83: Rituxan: key facts
• Table 84: Herceptin: key facts
• Table 85: Campath: key facts
• Table 86: Mylotarg: key facts
• Table 87: Bexxar: key facts
• Table 88: Avastin: key facts
• Table 89: Erbitux: key facts
• Table 90: Zevalin: key facts
• Table 91: Gleevec: key facts
• Table 92: Targretin: key facts
• Table 93: Iressa: key facts
• Table 94: Velcade: key facts
• Table 95: Tarceva: key facts
• Table 96: Ontak: key facts
• Table 97: Forecasts for antineoplastic monoclonalantibodies in the US, 2004-14
• Table 98: Forecasts for all other antineoplastics in theUS, 2004-14
• Table 99: Forecasts for marketed targeted therapies inJapan, 2004-14
• Table 100: Forecasts for marketed targeted therapies inFrance, 2004-14
• Table 101: Forecasts for marketed targeted therapies inGermany, 2004-14
• Table 102: Forecasts for marketed targeted therapies inItaly, 2004-14
• Table 103: Forecasts for marketed targeted therapies inSpain, 2004-14
• Table 104: Forecasts for marketed targeted therapies inthe UK, 2004-14
• Table 105: Forecasts for marketed targeted therapies inthe EU5, 2004-14
• Table 106: Global forecasts for antineoplasticmonoclonal antibodies, 2004-14
• Table 107: Global forecasts for all otherantineoplastics, 2004-14
• Table 108: Datamonitor drug assessment parameters
• Table 109: Abbreviations used in Pipeline/CommercialInsight: Innovative Targeted Therapies (1 of 2)
• Table 110: Abbreviations used in Pipeline/CommercialInsight: Innovative Targeted Therapies (2 of 2)

List of Figures

• Figure 1: Signal transduction inhibitors andangiogenesis inhibitors form the bulk of the 2005 targeted therapiespipeline
• Figure 2: A plethora of current early-phase agents willcome to light in the short-term future
• Figure 3: Targeting multiple tyrosine kinases appears tobe the current trend in R&D
• Figure 4: Targeting the primary VEGF receptor appearsthe most popular development strategy
• Figure 5: The majority of developmental agents affectunspecified apoptosis targets
• Figure 6: CDK appears to be the primary developmentaltarget for the cell cycle regulators
• Figure 7: The CD family of proteins appears mostfavorable for development
• Figure 8: Big four tumor types, plus melanoma and RCC,remain popular indications
• Figure 9: Hematological indications with the highestincidence dominate the developmental pipeline
• Figure 10: The majority of pipeline compounds are inearly-phase trials, therefore a high level of fragmentation exists
• Figure 11: Pipeline signal transduction inhibitors salesforecasts, 2005-14
• Figure 12: Pipeline angiogenesis inhibitors salesforecasts, 2005-14
• Figure 13: Pipeline apoptosis stimulators salesforecasts, 2005-14
• Figure 14: Pipeline HDAC inhibitors sales forecasts,2005-14
• Figure 15: Pipeline monoclonal antibodies salesforecasts, 2005-14
• Figure 16: Datamonitor drug assessment summary forpipeline signal transduction inhibitors
• Figure 17: Datamonitor drug assessment summary forpipeline angiogenesis inhibitors
• Figure 18: Datamonitor drug assessment summary forpipeline apoptosis stimulators
• Figure 19: Datamonitor drug assessment summary forpipeline HDAC inhibitors
• Figure 20: Datamonitor drug assessment summary forpipeline monoclonal antibodies
• Figure 21: Global oncology sales, 2002-09
• Figure 22: Oncology pipeline, 2003
• Figure 23: Forecast incidence of cancer across the sevenmajor markets, 2005-13
• Figure 24: Increasing combined incidence for breast,lung, prostate and colorectal cancer with increasing age, 2003
• Figure 25: Incidence increases, while the rate of cureand death reduces disease prevalence
• Figure 26: Point prevalence for colorectal and lungcancer differs markedly despite similar rates of incidence
• Figure 27: Unmet needs in cancer
• Figure 28: The process of tumor angiogenesis
• Figure 29: The multiple tyrosine kinase inhibitors willachieve the greatest commercial success
• Figure 30: The multiple tyrosine kinase inhibitorsappear most attractive in terms of research/clinical and commercialaspects
• Figure 31: PTK-787 is currently the front runner of theangiogenesis inhibitors due to the high patient potential of itsindication
• Figure 32: Candidates with the backing of key oncologyplayers appear most attractive among the pipeline angiogenesis inhibitors
• Figure 33: Genasense is the clear leader due to its widerange of developmental indications
• Figure 34: Route of administration may work against thepipeline apoptosis stimulators
• Figure 35: FK-228s sales are currently limited by itstarget indication
• Figure 36: A lack of clinical data and commercialexperience currently limit FK-228s attractiveness
• Figure 37: MLN-2704s commercial potential will increaseonce indications outside of prostate cancer are explored
• Figure 38: Attractiveness of MLN-2704 will increase oncedevelopment outside of prostate cancer is initiated
• Figure 39: Example of Datamonitor drug assessmentscorecard
• Figure 40: Example of Datamonitor drug assessment graph