Committed to innovation and growth Karl Mahler Head of Investor Relations Stefan Frings Oncology/Immunology Therapeutic Area Head Roche Partnering Roche Group June 2013
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Update on 2013 Strategy, R&D productivity and allocation of resources Oncology: ASCO 2013 Summary
Q1 2013: Strong start to the year 2013 2012 Change in % CHF bn CHF bn CHF CER Pharmaceuticals Division 9.2 8.6 6 7 Diagnostics Division 2.4 2.4 1 1 Roche Group 11.6 11.0 5 6 CER=Constant Exchange Rates 4
Q1 13: US and Emerging markets driving sales growth Pharma Diagnostics Asia 10% Asia- Pacific 10% Latin America 4% Latin America 7% EEMEA 11% US 13% North America -4% Japan 2% Japan -2% Europe 1% EMEA 1% All growth rates at CER=Constant Exchange Rates; EEMEA=Eastern Europe, Middle East, Africa; EMEA=Europe, Middle East and Africa 5
Update on 2013 Strategy, R&D productivity and allocation of resources Oncology: ASCO 2013 Summary
Premium for innovation Roche strategy: Focused on medically differentiated therapies Pharma Dia Regulators: Optimised benefit / risk ratio Focus Payors: Optimised benefit / cost ratio MedTech Generics OTC Differentiation 7
Personalised Healthcare - benefit for all stake holders, including the industry Today Benefit from patient stratification Future Reduced Patient pool Pricing power Increased market share Time to market Higher probability of success Lower development costs 8
Roche strategy: Tailor made access options for high value products Established Markets Emerging Markets Value based pricing Differential pricing Universal access and coverage -> Negotiate prices for new medicines Limited patient access -> Enable access to public funding 9
R&D productivity differs substantially among players Average annual NME peak sales (2001-10) 1 US$ bn $ 710 m Peak Sales (per $1 bn R&D) 4 x Roche $ 165 m Peak Sales (per $1 bn R&D) Average annual R&D investment (1997-2006) 1 US$ bn 1 Peak sales and R&D calculated pro forma to account for major M&A Source: EvaluatePharma; BCG analysis; Roche analysis 10
Roche: R&D well balanced from a risk & disease point of view 2012 Roche budget Oncology Metabolism Inflammation CNS Virology 0% 5% 10% 15% 20% 25% 30% Industry average probability of success Phase 0 to Registration Source: Bernstein Equity Research, Tufts University and Roche analysis 11
R&D spend: Balance between short and long term R&D spend by phase ~50% ~50% Invest for the future Invest for the near term Research/ Discovery Phase 0 Phase 1 Phase 2 Phase 3 Filing Phase 4 Note: Based on 2012 budget 12
Continued focus on external innovation Roche Partnering 150 existing partnerships ~ 35% of total R&D pipeline compounds (phase 1-3) are from external origin ~ 37% of total Pharma sales (2012) are from partnered compounds 13
low Medical differentiation high Implications of R&D productivity challenge Segregation will continue as only true innovation will be rewarded High differentiation Generics Me-too players?? True innovators No / limited differentiation low Willingness to pay for added value high 14
Update on 2013 Strategy, R&D productivity and allocation of resources Oncology: ASCO 2013 Summary
Roche oncology: one approval in 1 tumor type to 9 medicines in 14 tumor types Kadcyla Perjeta Erivedge Zelboraf Tarceva HER 2+ BC HER 2-positive BC Basal Cell Carcinoma Melanoma Pancreatic cancer Lung cancer Renal cancer Ovarian Recurrent glioblastoma Avastin Metastatic breast cancer Lung cancer Metastatic colorectal cancer Xeloda Colon cancer Colorectal cancer Breast cancer Gastric cancer HER2-positive gastric cancer Herceptin Early HER2-positive breast cancer HER2-positive metastatic breast cancer CLL MabTheraRituxan Indolent NHL Agressive NHL 1997 2005 2013
Best-in-class oncology pipeline 39 NMEs and 32 AIs supporting long-term growth Phase I (26 NMEs) MDM2 ant solid & hem tumors HER3 MAb solid tumors CSF-1R MAb solid tumors MEK inh solid tumors Tweak MAb oncology Ang2-VEGF MAb oncology Raf & MEK dual inh solid tumors CD44 MAb solid tumors MDM2 ant solid & hem tumors MEK inh solid tumors AKT inhibitor solid tumors PD-L1 MAb solid tumors Steap 1 ADC prostate ca. ADC ovarian ca. ADC multiple myeloma ADC oncology ADC oncology Bcl-2 inh CLL and NHL ChK1 inh solid tum & lymphoma PI3K inh solid tumors ADC metastatic melanoma PI3k inh glioblastoma 2L ChK1 inh(2) solid tumors ALK inhibitor NSCLC PI3K inh solid tumors WT-1 peptide cancer vaccine Phase II (8 NMEs+ 11 AIs) Perjeta BC neoadjuvant Perjeta HER2+ mbc 2 nd line Perjeta HER2+ gastric cancer Kadcyla (T-DM1) HER2+ gastric cancer Erivedge operable BCC onartuzumab triple-neg mbc, 1 st /2 nd line onartuzumab mcrc 1 st line onartuzumab NSCLC non squamous 1 st l onartuzumab NSCLC squamous 1 st line onartuzumab glioblastoma 2 nd line Zelboraf papillary thyroid cancer imgatuzumab (GA201) solid tumors pictilisib (PI3K inh) solid tumors PI3K/mTOR inh solid & hem tumors parsatuzumab (EGFL7 Mab) solid tumors CD22 ADC hem tumors CD79b ADC hem tumors HER3/EGFR m. epithelial tumors glypican-3 MAb liver cancer Phase III (3 NMEs+17 AIs) Avastin HER2+ BC adj Avastin HER2-neg. BC adj Avastin NSCLC adj Avastin high risk carcinoid Avastin 1 ovarian cancer 1 st line Avastin 1 rel. ovarian ca. Pt-resistant Avastin 1 rel. ovarian ca. Pt-sensitive Perjeta HER2+ early BC Tarceva NSCLC adj Kadcyla (T-DM1) HER2+ mbc 3 rd line Kadcyla (T-DM1) HER2+ mbc 1 st line Kadcyla (T-DM1) HER2+ early BC onartuzumab gastric cancer obinutuzumab inhl relapsed obinutuzumab DLBCL obinutuzumab inhl front-line Zelboraf m. melanoma adj onartuzumab NSCLC 2 nd /3 rd line obinutuzumab CLL cobimetinib (MEKinh) m. melanoma Registration (2 NMEs+4 AIs) MabThera 2 NHL sc formulation Avastin 2 glioblastoma 1 st line Herceptin 2 HER2+ BC sc form Tarceva 4 NSCLC EGFR mut 1 st line Kadcyla 3 (T-DM1) HER2+ pretr. mbc Erivedge 3 advanced BCC 1 US only: ongoing evaluation for FDA submission 2 Submitted in EU 3 Approved in US, submitted in EU 4 Approved in EU, submitted in US New Molecular Entity (NME) Additional Indication (AI) Status as of March 31, 2013 17
R&D cycle: Translating learnings from the clinic into preclinical research Learn in the lab: Learn in the clinic: Bedside to bench 18
Improving cancer treatment with combinations 29 internal combinations with 18 compounds in over 9 tumor types, and increasing Solid tumors Breast cancer Perjeta Perjeta Lung cancer Herceptin Herceptin Kadcyla Perjeta Ph3 Kadcyla Perjeta Ph3 Perjeta Herceptin Ph3 Onartuzumab Avastin Ph2 Pictilisib (PI3Ki) Kadcyla Ph1 Pictilisib (PI3Ki) Herceptin Ph1 Onartuzumab Tarceva Ph3 Onartuzumab Avastin Ph2 Anti-EGFL7 Avastin Ph2 Pictilisib (PI3Ki) Avastin Ph2 Pictilisib (PI3Ki) Avastin Ph1 Pictilisib (PI3Ki) Tarceva Ph1 Colon cancer Onartuzumab Avastin Ph2 Anti-EGFL7 Avastin Ph2 Anti-PDL1 Avastin Ph1 Melanoma Cobimetinib Zelboraf Ph3 Anti-PDL1 Zelboraf Ph1 Gastric, brain, kidney and others Perjeta Herceptin Ph3 Onartuzumab Avastin Ph2 Anti-PDL1 Avastin Ph1 Cobimetinib AKT inh Ph1 Cobimetinib Pictilisib (PI3Ki) Ph1 Anti-HER3 MAb Tarceva Ph1 Hematological tumors Lymphoma Anti-CD22 ADC Rituxan Ph2 Anti-CD79b ADC Rituxan Ph2 Bcl2 inh Rituxan (+B) Ph1 Leukemia Bcl2 inh GA101 Ph1 Bcl2 inh Rituxan Ph1 Bcl2 inh Rituxan (+B) Ph1 Studies read out/filed/approved 19
Medical value Strategies beyond great medicines HER2 franchise Replace and extend Replace Extend Perjeta Perjeta Kadcyla Kadcyla Herceptin + chemo Lapatinib + chemo Herceptin + chemo EMILIA / MARIANNE CLEOPATRA MARIANNE 20
Changing the standard of care in HER2 Securing future growth by improving the standard of care Biosimilars launch (EU) 2nd line mbc Xeloda + lapatinib T-DM1 (EMILIA) 1st line mbc Herceptin + chemo Herceptin & Perjeta + chemo (CLEOPATRA) T-DM1 & Perjeta (MARIANNE) Adjuvant BC Herceptin + chemo Herceptin subcutaneous + chemo (HannaH) Herceptin & Perjeta + chemo (APHINITY) T-DM1 & Perjeta + chemo 2011 2012 2013 2014 2015 2016 2017 2018 2019 2020 Filing timelines Established standard of care Potential new standard of care Potential future standard of care 21
Changing the standard of care in hematology Different mechanisms of action MabThera Rituxan* GA 101 Filed in Q2 2013 and received breakthrough designation by FDA 2012 2014 2016 2018 2020 Bcl-2 Anti-CD22 ADC or Anti-CD79b ADC * Patent expiry in the US: 2018 22
Medical value Strategies beyond great medicines Hematology Replace and extend Replace Extend BCL2 ADCs BCL2 ADCs ADC 22 ADC 79b GA101 Chemo ADC 22 ADC 79b GA101 MabThera MabThera CLL11 etc. Romulus Our vision 23
Progression-free survival GA101 in CLL: Investigator-assessed PFS (months) Stage Ia Stage Ib 1.0 0.9 0.8 G-Clb: Median 23.0 mo* 1-year PFS 84% 1.0 0.9 0.8 R-Clb: Median 15.7 mo 1-year PFS 63% 0.7 0.7 0.6 0.6 0.5 0.4 0.3 Clb: Median 10.9 mo 1-year PFS 27% 0.5 0.4 0.3 Clb: Median 10.8 mo 1-year PFS 27% 0.2 0.1 0.0 Stratified HR: 0.14 95% CI: 0.09 0.21 p < 0.0001 (log-rank) 0 3 6 9 12 15 18 21 24 27 n at risk Clb 118 99 82 47 18 5 3 0 0 0 G-Clb 238 213 207 152 117 75 40 15 2 0 0.2 0.1 0.0 Stratified HR: 0.32 95% CI: 0.24 0.44 p < 0.0001 (log-rank) 0 3 6 9 12 15 18 21 24 27 Clb 118 101 85 49 19 6 3 0 0 0 R-Clb 233 225 215 148 95 63 28 11 3 0 Type 1 error controlled through closed test procedure; p-value of the global test was <.0001. * In the G-Clb arm < 10% of patients had reached the median at cutoff; therefore, in contrast to the Clb arm the G-Clb median PFS could not be reliably estimated due to the few patients at risk at time of G-Clb median. Independent Review Committee (IRC) - assessed PFS was consistent with investigator-assessed PFS 24 CI = confidence interval; HR = hazard ratio.
GA101 in NHL: Phase III development GADOLIN study Rituximab-refractory inhl (n=360) Induction GA101 + bendamustine x 6 cycles Bendamustine x 6 cycles CR, PR, SD Maintenance GA101 q2mo x 2 years Primary end-point: PFS Expect data: 2015 GOYA study Previously untreated DLBCL (n=1,400) GA101 x 8 cycles + CHOP x 6 or 8 MabThera x 8 cycles + CHOP x 6 or 8 Primary end-point: PFS Expect data: 2015 GALLIUM study First-line inhl (n=1,400) Induction GA101 x 8 cycles + CHOP x 6 or GA101 x 8 cycles + CVP x 8 or GA101 x 6 cycles + benda. x 6 MabThera x 8 cycles + CHOP x 6 or MabThera x 8 cycles + CVP x 8 or MabThera x 6 cycles + benda. x 6 CR, PR Maintenance GA101 q2mo x 2 years MabThera q2mo x 2 years Primary end-point: PFS Expect data: 2017 25
Tumor PD-L1 enables cancer immune evasion Anti-PDL1 inhibits binding of PD-L1 to PD-1 and B7.1 Targeting PDL1 Targeting PD-1 26
Selecting the patients most likely to benefit Companion diagnostics Anti-PDL1 immunohistochemistry (proprietary Genentech/Roche PD-L1 IHC) Companion diagnostics factors Highly sensitive and specific anti-pdl1 antibody used for IHC PD-L1 expression on tumor cells PD-L1 PD-L1 expression on tumor infiltrating immune cells Appropriate diagnostic cut-off T cell Prospective evaluation of diagnostic cancer cell 27
Anti-PDL1: Phase I data in solid tumors Efficacy Overall Phase I experience Metastatic NSCLC Metastatic Melanoma Metastatic RCC Response rates 1 All comers 2 Dx-positive 3 21% (29/140) 22% (9/41) 29% (11/38) 13% (6/47) 36% (13/36) 80% (4/5) 27% (4/15) 20% (2/10) 26 of 29 responders continued to respond at last assessment (time on study of 3 to over 15 months) Safety Grade 3/4 adverse events % (n) All Grade 3/4 Events 43% (73/171) Hyperglycemia 5% (9/171) No grade 3-5 pneumonitis observed Immune-related Grade 3-4 AEs observed in 4 patients (2%) Treatment-related Grade 3-4 AEs in 22 patients (13%) Fatigue 4% (7/171) Increased ALT 3% (5/171) Dyspnea 3% (5/171) Hypoxia 3% (5/171) 28 1 Efficacy evaluable subjects first dosed at 1-20 mg/kg prior to Aug 1, 2012; data cutoff Feb 1, 2013; ORR includes unconfirmed PR/CR and confirmed PR/CR by RECIST 1.1 2 All patients include PD-L1-positive, PD-L1-negative and patients with unknown tumor PD-L1 status; 3 Diagnostic positivity based on Roche PD-L1 IHC
Patients, % Anti-PDL1: Disease control rate Phase I Overall disease control rate Disease control rate by tumor type 100 Disease Control Rate (ORR 1 + SD) 80 60 40 20 0 50 41 28 33 13 20 PD-L1 positive PD-L1 negative All comers Overall Phase I experience Metastatic NSCLC Metastatic Melanoma Metastatic RCC All comers 1 Dx-positive 2 61% (86/140) 54% (22/41) 58% (22/38) 72% (34/47) 86% (31/36) 100% (5/5) 87% (13/15) 80% (8/10) Best response: Complete response Partial response Stable disease 29 1 All patients include PD-L1-positive, PD-L1-negative and patients with unknown tumor PD-L1 status; 2 Diagnostic positivity based on Roche PD-L1 IHC
Anti-PDL1: Salvage of BRAF-mutant metastatic melanoma patient after progression on Zelboraf Baseline Week 6 Week 12 Week 18 31% increase in target lesions (RECIST PD) Post-Resection Dx: Nov 2010 (cutaneous melanoma) Prior treatment: cisplatin, vemurafenib. Week 46 Images include data from after Feb 1, 2013 Dana Farber Cancer Institute (Ibrahim/Hodi). 30
Update on 2013 Strategy, R&D productivity and allocation of resources Oncology: ASCO 2013 Summary
Q1 2013: Pipeline milestones aleglitazar metabolic diseases lebrikizumab asthma mglur2 antagonist treatment-resistant depression gantenerumab 1 Alzheimer s mglur5 antagonist treatment-resistant depression ocrelizumab MS crenezumab Alzheimer's bitopertin schizophrenia Anti-PD-L1* solid tumours HCV combo HepC MEKi melanoma Anti-EGFL7 solid tumours etrolizumab ulcerative colitis Oncology onartuzumab (MetMAb) NSCLC obinutuzumab (GA101) * CLL Kadcyla HER2+ BC EGFR ADCC MAb (GA201) solid tumours PI3 kinase solid tumours dual PI3 kinase/mtor solid tumours Anti-factor D geographic atrophy Anti-PCSK9 metabolic diseases inclacumab (P selectin)* ACS/CVD Neuroscience Virology Immunology Ophthalmology Metabolism Ph III NMEs Late stage enabling data expected in 2013 *Data presentation planned/presented 1 Phase II/III label enabling 2013 R&D to remain stable 32
NME submissions and their additional indications Projects currently in phase 2 and 3 obinutuzumab (GA101) Frontline DLBCL NHL obinutuzumab (GA101) Frontline NHL onartuzumab (MetMAb) gastric cancer & other AIs etrolizumab (RG7413) ulcerative colitis quilizumab (RG7449) asthma lebrikizumab (RG3637) asthma obinutuzumab (GA101) CLL onartuzumab (MetMAb) mnsclc, 2 nd /3 rd line cobimetinib (MEK inh) (RG7421) combo Zelboraf met melanoma octreolin (RG3806) acromegaly obinutuzumab (GA101) inhl relapsed aleglitazar type-2 diabetes (US/China) aleglitazar (RG1439) CV risk red post ACS in T2D bitopertin (RG1678) schizophrenia# ocrelizumab (RG1594) PPMS and RMS imgatuzumab EGFR (RG7160) solid tumors pictilisib PI3 kin inh (RG7321) solid tumors PI3K/mTOR inh (RG7422) solid & hem tumors parsatuzumab EGFL7 MAb (RG7414) solid tumors CD22 ADC (RG7593) CD79b ADC (RG7596 heme tumors HER3/EGFR (RG7597) m. epithelial tumors glypican-3 MAb (RG7686) liver cancer RG7667 CMV mericitabine (RG7128) HCV danoprevir (RG7227) HCV setrobuvir (RG7790 ) HCV aleglitazar (RG1439) CV risk red CVD in T2D/pre-T2D inclacumab (RG1512) ACS/CVD PCSK9 MAb (RG7652) metabolic diseases 2013 2014 2015 2016 and beyond bitopertin (RG1678) obsessive compulsive dis. gantenerumab (RG1450) Alzheimer s MAO-B inh (RG1577) Alzheimer s mglur2 antag (RG1578) depression mglur5 (RG7090) depression crenezumab (RG7412) Alzheimer s lampalizumab anti-factor D Fab (RG7417) geographic atrophy Unless stated otherwise, submissions are planned to occur in US and EU. indicates a submission which has occurred with regulatory action pending # negative symptoms and sub-optimal control Status as of March 31, 2013 Oncology Immunology Virology CardioMetabolism Neuroscience Ophthalmology NME 33
Summary: Focus on innovation and growth 1 Strategic focus on innovation and driving Personalised Healthcare 2 Strong growth in US and Emerging Markets; innovative access models 3 Leading product pipeline providing value for the future 34
Doing now what patients need next