P Fumoleau, 1 A Wardley, D Miles, S Verma, K Gelmon, D Cameron, L Gianni, PF Conte, G Ross, V McNally, J Baselga

1. Safety of pertuzumab plus trastuzumab in a Phase II trial of patients with HER2-overexpressing metastatic breast cancer which had progressed duringtrastuzumab therapy P Fumoleau,1 A Wardley, D Miles, S Verma, K Gelmon, D Cameron, L Gianni, PF Conte, G Ross, V McNally, J Baselga 1Centre Georges-François-Leclerc, Dijon, France

2. Pertuzumab background • Pertuzumab, a humanized monoclonal antibody, is a HER2 dimerization inhibitor • HER2 is the preferred co-receptor for HER1, HER3 and HER4 dimers • HER signaling is implicated in cancer cell proliferation and survival • Pertuzumab inhibits both HER2 homodimerization and heterodimerization, blocking multiple HER signaling pathways HER, human epidermal growth factor receptor

3. Rationale for this study • Pertuzumab and trastuzumab bind distinct and non-overlapping epitopes of HER2 • The addition of pertuzumab post-progression to ongoing trastuzumab in xenografts synergistically increased tumor inhibition compared with trastuzumab alone • Patients with disease progression during trastuzumab treatment have high unmet need • An understanding of the adverse event profile of this combination, particularly cardiac safety, is of importance

4. YES NO Study design Simon-type two-stage design Stage 2 (n=66) ≥2 R or 1 R + 12 SDor 13 SD Safety evaluationfor IDSMB Stage 1 (n=24)Trastuzumab +pertuzumaba Stop trial • There have been no safety objections raised by the IDSMB regarding continuing the study into stage 2 • n=58 fully evaluable patients needed aTrastuzumab: 4 mg/kg loading dose  2 mg/kg qw or 8 mg/kg loading dose  6 mg/kg q3w;Pertuzumab: 840 mg loading dose  420 mg q3w IDSMB, International Data Safety Monitoring Board

5. Main eligibility criteria • Up to 3 lines of prior cytotoxic therapies and / or trastuzumab (including in the adjuvant setting) • Disease progression during trastuzumab as most recent treatment for metastatic disease • No brain metastases • Baseline LVEF ≥55% • No decrease of LVEF to <50% during prior trastuzumab treatment • Within 9 weeks of last trastuzumab treatment LVEF, left ventricular ejection fraction

6. Recruitment end 10 July, 2007 Patientsenrolled 70 Stage 2: 39 patients have received treatment 60 50 Stage 1: 27 patients have received treatment 40 30 20 Planned cumulative 10 Actual cumulative 0 Mar06 Apr06 May06 Jun06 Jul06 Aug06 Sep06 Oct06 Nov06 Dec06 Jan07 Feb07 Mar07 Apr07 May07 Jun07 Jul07 Study fully recruited • Efficacy population n=33 • all patients who received 2 cycles of study treatment and an end of cycle 2 tumor assessment at April ASCO snapshot (no other planned efficacy cuts) • Safety population n=61 • all patients randomized and received study treatment at last IDSMB snapshot in August

7. Safety population • 61 patients had received at least one dose of study medication at thetime of the data cut-off • all 61 patients are included in the safety population • median cycles received = 4 • range of cycles received = 1-16 • 64% of patients received prior anthracyclines

8. Patient characteristics Characteristic No. patients No. patients Age (years), median (range) ECOG performance status 0 / 1 (%) Organ site (target and non-target lesions), n (%) Visceral Lung Liver Bone Lymph nodes Soft tissue Other ER status (%) +ve / -ve Total lesions (target and non-target), median (range) 61 54 (25-85) 70 / 16 48 (78) 24 (39) 32 (53) 16 (26) 24 (39) 10 (16) 7 (11) 48 / 51 3.5 (1-14) ECOG, Eastern Cooperative Oncology Group; ER, estrogen receptor

9. All adverse events Adverse event (AE) Diarrhea Skin (other than rash) Nausea / vomiting Mucositis Pain Rash Fatigue Deep vein thrombosis (DVT), ejection fraction decreased, hypersensitivity, hypertension, hypomagnesemia Incidenceall grades (%) n=61 35 (59) 19 (31) 22 (36) 20 (33) 26 (43) 18 (30) 17 (28) 1 each (2) IncidenceGrade 3 / 4 (%) 1 (2) 0 (0) 0 (0) 0 (0) 0 (0) 1 (2) 0 (0) 1 DVT (2)

10. Treatment-related adverse events: grade ≥3 Adverse event(n=1; 2%) Diarrhea Grade 3 Outcome Resolved Treatmentcontinued Yes

11. Aftercycle 1 n= 54 Aftercycle 2 n= 51 Aftercycle 4 n= 35 Aftercycle 6 n= 23 Aftercycle 8 n= 14 Aftercycle 12 n= 10 Summary of the mean change in LVEF from baseline over time: local reading Baseline mean: 61.1% (SEM 0.67); median 60.0% (range 51-75) Mean absolute change in LVEF (%)

12. Summary of LVEF data over time: local reading Baseline mean: 61% (SD 5.17); median 60.0% (range 51-75) Aftercycle 1 2 4 6 8 12 16 n 54 51 35 23 14 10 4 Increase, n/c,or change ≤10% 53 (98%) 50 (98%) 34 (97%) 22 (96%) 13 (93%) 9 (90%) 4 (100%) ≤50% &≥10% 1 (2%) ≤50% &≥15% Othera 1 (2%) 1 (3%) 1 (4%) 1 (7%) 1 (10%) aReading taken but the result invalid

13. Patient with falling LVEF(local vs central reading) • Only 2 patients had a falling LVEF (≤50% and ≥10%) • Patient 1 remained asymptomatic; withdrawn from study at cycle 3 for disease progression Cycle Patient 1 Screening 1 2 Final visit LVEFLocala 56 50 42 42 LVEFCentralb 63 56 56 54 Changefrom baselinea -6% -14% -14% Changefrom baselineb -6.4% -6.6% -8.8% aLocal reading (patients managed according to local reading); bCentral reading

14. Patient with falling LVEF(local vs central reading) • Only 2 patients had a falling LVEF (≤50% and ≥10%) • Patient 2 remained asymptomatic; withdrawn from study at the end of cycle 4 for disease progression Cycle Patient 2 Screening 1 2 4 LVEFLocala 60 56 60 55 LVEFCentralb 71 53 46 70 Changefrom baselinea -4% 0% -5% Changefrom baselineb -18% -25% -1% aLocal reading (patients managed according to local reading); bCentral reading

15. Interim efficacy data as presented at ASCO 07 • n=33 • Overall response rate = 18.2% • Clinical benefit rate = 39.4% • Efficacy results updated for all 66 patients in trial will be reported in 2008 Baselga et al ASCO 2007

16. CLEOPATRA : Phase III studyof trastuzumab + pertuzumab in HER2+ MBC Trastuzumab + docetaxel + placebo 1:1 randomization HER2+ MBC n = 800 Trastuzumab + docetaxel + pertuzumab An international Phase III randomized, double-blind, placebo-controlled study (approximately 250 sites worldwide) • Endpoints: • Progression-free survival • Overall survival • Quality of life • Biomarker analysis

17. Neoadjuvant trastuzumab and pertuzumab HER2+ LABC and large stage II breast cancer (n=400) Trastuzumab + pertuzumab + docetaxelq3w x 4 Trastuzumab + docetaxelq3w x 4 Trastuzumab + pertuzumabq3w x 4 Pertuzumab + docetaxelq3w x 4 Surgery Surgery Surgery Surgery FEC q3w x 3 trastuzumab q3w until Week 52 FEC q3w x 3 trastuzumab q3w untilWeek 52 FEC q3w x 3 trastuzumab q3w untilWeek 52 Docetaxel + trastuzumab q3wx 4 FEC q3w x 3 trastuzumab q3w until Week 52 • Endpoints: • pCR • Biomarker analysis

18. Conclusions • Pertuzumab is a promising agent with a new mechanism of action • Pertuzumab plus trastuzumab is active and well tolerated in patients with HER2-positive breast cancer • No significant cardiac events have been observed in 61 patients in this study • The trial is ongoing, with an additional pertuzumab monotherapy arm