Transcript Lapatinib
19th Annual NOCR Meeting Session I: Breast Cancer HER-2+ Disease Christy A Russell, MD Keck School of Medicine University of Southern California HER-2+ Breast Cancer • Adjuvant and Neoadjuvant Therapy • Combining Trastuzumab with other HER2directed agents • Second generation choices • Novel agents and conjugates Signal Transduction by the HER Family and Potential Mechanisms of Action of Trastuzumab Hudis C. N Engl J Med. 2007;357:39-51. Metastatic Breast Cancer Front-line Options Trastuzumab Combinations as First-line Therapy for MBC: Pivotal Phase III Trial Paclitaxel Patients with HER2+ (IHC 2+/3+) MBC, no previous chemotherapy, measurable disease, KPS ≥ 60% (N = 469) Previous adjuvant AC (n = 96) Trastuzumab + Paclitaxel (n = 92) AC No previous adjuvant AC (n = 138) Trastuzumab + AC (n = 143) Slamon DJ, et al. N Engl J Med. 2001;344:783-792. Trastuzumab in MBC: The Pivotal Trial Treatment Objective Response Rate, % Median TTP, Mos Median OS, Mos Chemo 32 4.6 20.3 Chemo + Trastuzumab 50 7.4 25.1 P < .001 for all comparisons. Slamon DJ, et al. N Engl J Med. 2001;344:783-792. Trastuzumab in Recommended First-line Combinations for HER2+ MBC • HER2+ disease without previous trastuzumab: trastuzumab plus – Paclitaxel ± carboplatin – Docetaxel – Vinorelbine – Capecitabine NCCN. Clinical practice guidelines in oncology: breast cancer. v2.2011. Trastuzumab in Triple-Combination Regimens: Response Rates Yardley et al, 2004 (N = 24) H+V+T Untch et al, 2004 (N = 25) H + E90 + C Untch et al, 2004 (N = 26) H + E60 + C Dirix et al, 2006 (N = 34) H + Carbo + T Chan et al, 2007 (N = 34) H+V+X Fountzilas et al, 2004 (N = 40) H+G+P Yardley et al, 2006 (N = 41) H + G + Carbo Miller et al, 2002 (N = 45) H+G+P Venturini et al, 2006 (N = 45) H+E+T Perez et al, 2005 (N = 43) H + Carbo + P every 3 wks Perez et al, 2005 (N = 48) H + Carbo + P every wk Cortes et al, 2004 (N = 54) H + TLC D-99 + P Yardley et al, 2002 (N = 61) H + Carbo + T Pegram et al, 2004 (N = 59) H + Carbo + T Pegram et al, 2004 (N = 62) H + Cisplatin + T Robert et al, 2006 (N = 92) H + Carbo + P Wardley et al, 2006 (N = 111) H+X+T Forbes et al, 2006 (N = 130) H + Carbo + T 0 10 20 30 40 50 ORR (%) 60 70 80 90 100 Hormonal Therapy in HER2+ MBC Regimen ORR, % PFS, Mos Trastuzumab (N = 79)[1] 26 3.5-3.8 Anastrozole + trastuzumab (N = 103)[2] 20 4.8 Anastrozole (N = 104)[2] 7 2.4 Lapatinib + letrozole (N = 642)[3] 28 8.2 Letrozole (N = 644)[3] 15 3.0 Lapatinib (N = 138)[4] 24 NA 1. Vogel C, et al. J Clin Oncol. 2002;20:719-726. 2. Mackey JR, et al. SABCS 2006. Abstract 3. 3. Johnston S, et al. J Clin Oncol. 2009;27:5538-5546. 4. Gomez HL, et al. J Clin Oncol. 2008;26:2999-3005. Mechanism of Action of Lapatinib Compared to Trastuzumab Trastuzumab T 1 1 2 2 1 2 L L L L L L Erb receptors Downstream signaling pathways Cell proliferation Cell survival Lapatinib Lapatinib as First-line Treatment for HER2Amplified LABC or MBC Patients (N = 138) randomized to 2 schedules of lapatinib monotherapy Endpoint Lapatinib 1500 mg/day (n = 69) Lapatinib 500 mg BID (n = 69) All Patients (N = 138) Response rate, n (%) 15 (22) 18 (26) 33 (24) Clinical benefit rate, n (%) 20 (29) 23 (33) 43 (31) 41 45 43 6-mo PFS, % Median time to response (all patients): 7.9 wks; median duration of response (all patients): 28.4 wks Safety: only grade 1/2 asymptomatic cardiac adverse events (4 patients) Gomez HL, et al. J Clin Oncol. 2008;26:2999-3005. Trastuzumab vs Lapatinib First-Line Therapy for MBC MA.31/EGF108919: Design Randomize Experimental Arm 24 Wks: Lapatinib + taxane Standard Arm Until PD: Lapatinib 24 Wks: Trastuzumab + taxane Until PD: Trastuzumab Primary Outcome: PFS Sample size: ~ 600 (536 patients centrally confirmed with HER2+) ClinicalTrials.gov. NCT00667251. Gelmon, ASCO 2012 [TITLE] NCCN: Treatment of HER2+ MBC Beyond First Line With Previous Trastuzumab Exposure • Continued HER2 blockade – Chemotherapy + trastuzumab – Trastuzumab + lapatinib – Capecitabine + lapatinib NCCN. Clinical practice guidelines in oncology: breast cancer. v.3.2012. EGF100151 Phase III Study: Lapatinib + Capecitabine in Advanced Breast Cancer Patients with HER2+ progressive MBC or stage IIIB/IIIC LABC with T4 lesion and unlimited previous therapies* Lapatinib 1250 mg/day PO + Capecitabine 2000 mg/m2/day on Days 1-14 every 21 days Capecitabine 2500 mg/m2/day on Days 1-14 every 21 days Primary endpoint: TTP Secondary endpoints: OS, PFS, ORR *No previous capecitabine and must have included trastuzumab (MBC) or anthracycline/taxane (MBC or adjuvant). Geyer C, et al. N Engl J Med. 2006;355:2733-2743. 100 TTP With 1 Previous Trastuzumab Regimen 80 Capecitabine Lapatinib + capecitabine 60 40 20 0 0 20 40 Wks 60 80 Cumulative Progression Free (%) Cumulative Progression Free (%) Lapatinib + Capecitabine in HER2+ MBC: TTP TTP With > 1 Previous Trastuzumab Regimen 100 80 Capecitabine Lapatinib + capecitabine 60 40 20 0 0 20 40 Wks 60 Reproduced with permission of The Oncologist, from Lapatinib plus capecitabine in women with HER-2–positive advanced breast cancer: Final survival analysis of a phase III randomized trial, Cameron D, et al., Vol 15, 2010; permission conveyed through Copyright Clearance Center, Inc. Cameron D, et al. Oncologist. 2010;15:924-934. 80 Lapatinib + Capecitabine in HER2+ MBC: Efficacy Result Capecitabine (n = 201) Capecitabine + Lapatinib (n = 207†) HR P Value Median TTP, wks[1] 18.6 31.3 0.50 < .001 OS, wks[1] 56.6 71.4 0.79 .077 ORR, %[2] 13.9 23.7 -- .017 13 (6) 4 (2) -- .045 Brain mets as site of first progression,* n (%)[2] † n=198 in 2008 study. *Exploratory analysis. 1. Cameron D, et al. Oncologist. 2010;15:924-934 2. Cameron D, et al. Breast Cancer Res Treat. 2008;112:533-543. Tumor Volume (mm3) Combining Lapatinib and Trastuzumab Increases Antitumor Activity 1600 1400 1200 1000 800 Control Trastuzumab Lapatinib Trastuzumab + lapatinib * * †‡ 600 400 200 † † § 0 13 16 19 21 23 Days After Injection *P < .05; †P < .01 vs control; ‡P < .05 vs trastuzumab; §P < .01 vs both lapatinib and trastuzumab. – Effect was durable: no tumor relapse observed at 8 mos after treatment Lapatinib induced accumulation of inactive HER2 at plasma membrane – Trastuzumab-mediated cytotoxicity was higher with the addition of lapatinib in MCF7/HER2 cells Reprinted by permission from Macmillan Publishers Ltd: Oncogene; Scaltriti, et al. 28:803-814, copyright 2009. Treatment with lapatinib plus trastuzumab resulted in complete tumor remission in mouse model In vivo activity was consistent with in vitro data demonstrating the combination as synergistic Scaltriti M, et al. Oncogene. 2009;28:803-814. Konecny GE, et al. Cancer Res. 2006;66:16301639. Xia W, et al. Oncogene. 2004;23:646-653. Pivotal Trial EGF104900 Lapatinib 1500 mg/day PO Patient Population HER2+ MBC Multiple lines of trastuzumab Progression on trastuzumab at study entry R Crossover at the time of progressive disease Lapatinib 1000 mg/day PO + trastuzumab 4 mg/kg then 2 mg/kg IV q wk Primary endpoint: PFS Secondary endpoints: OS, ORR, CBR Blackwell KL, et al. J Clin Oncol. 2012;30:2585-2592. Lapatinib ± Trastuzumab in MBC: PFS Outcome Lapatinib (n = 145) Lapatinib/ Trastuzumab (n = 146) HR (95% CI) P Value 6-mos PFS, % 13 28 0.73 (0.57-0.93) .008 Progressed or died, n 128 127 -- -- Median PFS, wks 8.1 12.0 -- -- Blackwell KL, et al. J Clin Oncol. 2010;28:1124-1130. EGF104900: Overall Survival L+T (n = 148) L (n = 148) n 146 145 Median OS, mos 14.0 9.5 100 80% Survival(%) 80 HR (95% CI) 70% 60 56% 6-mo OS 40 0.74 (0.57-0.97) Stratified log-rank P value .026 52% of patients in the L arm crossed over to L + T 41% 12-mo OS 20 0 0 Pts at risk, n Lap 1000/Tras 146 Lap 1500 145 5 120 100 10 25 15 20 Mos From Randomization 30 87 64 1 Blackwell KL, et al. J Clin Oncol. 2012;30:2585-2592. 63 46 42 28 25 13 35 Trastuzumab Beyond Progression in HER2+ MBC: BIG 03-05 Phase III Trial Patients with progressive MBC or LABC, HER2 overexpression, previous trastuzumab within 6 wks, and LVEF ≥ 50 (N = 156*) Primary endpoint: TTP Trastuzumab 6 mg/kg every 3 wks + Capecitabine 2500 mg/m2/day on Days 1-14 every 21 days (n = 78) Capecitabine 2500 mg/m2/day on Days 1-14 every 21 days (n = 78) Secondary endpoints: OS, ORR, safety *Study closed at 156 patients due to slow accrual following FDA approval of lapatinib for this indication. von Minckwitz G, et al. J Clin Oncol. 2009;27:1999-2009. BIG 03-05: Trastuzumab Beyond Progression in HER2+ MBC PFS X XH Censored Log-rank P = .0338 Probability of PFS 0.8 OS 1.0 0.6 0.4 0.2 X XH Censored Log-rank P = .2570 0.8 Probability of OS 1.0 0.6 0.4 0.2 0 0 0 10 20 Mos 30 40 0 10 Pts at Risk, n Pts at Risk, n X 74 40 15 8 5 3 2 1 1 X 74 66 50 33 XH 77 55 29 12 4 3 1 1 1 XH 77 68 59 47 Reprinted with permission. © 2008 American Society of Clinical Oncology. All rights reserved. von Minckwitz G, et al. J Clin Oncol. 2009;27:1999-2009. 20 Mos 21 27 30 10 15 3 6 40 3 1 2 1 New Option in the Front-Line: Pertuzumab Pertuzumab and Trastuzumab: Mechanisms of Action Pertuzumab HER2 Trastuzumab HER1/3/4 Dimerization domain Subdomain IV Trastuzumab: Inhibits ligand-independent HER2 signaling Activates ADCC Prevents HER2 ECD shedding Pertuzumab: Inhibits ligand-dependent HER2 dimerization and signaling Activates ADCC Ferguson KM, et al. Mol Cell. 2003;11:507-517. Olayioye MA, et al. EMBO J. 2000;19:3159-3167. Hynes NE, et al. Nat Rev Cancer. 2005;5:341-354. Rowinsky EK. Annu Rev Med. 2004;55:433-457. Phase II Trial of Pertuzumab + Trastuzumab in HER2+ MBC: Efficacy 60 SD PR CR Patients (%) 50 40 Responses were durable: Median duration of response: 5.8 mos Median PFS (all patients): 5.5 mos 30 20 10 0 All Patients (N = 66) Baselga J, et al. J Clin Oncol. 2010;28:1138-1144. CLEOPATRA Study Design Docetaxel (≥ 6 cycles recommended) Centrally confirmed HER2positive locally recurrent, unresectable or MBC N = 406 Trastuzumab ≤ 1 hormonal regimen for MBC Prior (neo)adjuvant systemic Rx, including trastuzumab and/or taxane allowed if followed by DFS ≥ 12 mos R Baseline LVEF ≥ 50%; no CHF or LVEF < 50% during or after previous trastuzumab Placebo 1:1 Docetaxel (≥ 6 cycles recommended) Trastuzumab N = 402 Pertuzumab Primary endpoint: Independently assessed PFS Baselga J, et al. N Engl J Med. 2012;366:109-119. CLEOPATRA: Progression-Free Survival Independently Assessed Median PFS Pertuzumab, Mos (n = 402) Placebo, Mos (n = 406) HR P Value 18.5 12.4 0.62 < .001 Baselga J, et al. N Engl J Med. 2012;366:109-119. CLEOPATRA: Overall Survival (Confirmatory Analysis) Pertuzumab, % Placebo, % (n = 402) (n = 406) Median OS, mos NR Swain SM, et al. SABCS 2012. Abstract P5-18-26. 37.6 HR P Value 0.66 .0008 CLEOPATRA: Safety Results Select Adverse Events (Grade ≥ 3), % Pertuzumab Placebo (n = 407) (n = 397) Neutropenia 48.9 45.8 Febrile neutropenia 13.8 7.6 Leukopenia 12.3 14.6 Diarrhea 7.9 5.0 Peripheral neuropathy 2.7 1.8 Left ventricular systolic dysfunction 1.2 2.8 Baselga J, et al. N Engl J Med. 2012;366:109-119. NCCN: First-line Treatment of HER2+ MBC With No Previous Trastuzumab Exposure Preferred regimens – Docetaxel + trastuzumab + pertuzumab (category 1) – Paclitaxel + trastuzumab + pertuzumab Other regimens – Chemotherapy + trastuzumab NCCN. Clinical practice guidelines in oncology: breast cancer. V.1.2013. Second-line and Further Therapy TDM-1 Trastuzumab/Emtansine: Novel Antibody– Drug Conjugate Target expression: HER2 Monoclonal antibody: trastuzumab Trastuzumab Cytotoxic agent: emtansine (DM1) Highly potent cytotoxic agent DM1 MCC Linker: SMCC T-DM1 Systemically stable Average drug:antibody ratio ≅ 3.5:1 EMILIA Phase III Study: T-DM1 vs Lapatinib/Capecitabine in HER2+ MBC Stratified by world region, number of previous chemotherapy regimens for MBC or unresectable locally advanced breast cancer, presence of visceral disease Patients with HER2-positive locally advanced or MBC* (N = 980) *All pts received previous taxane and trastuzumab T-DM1 3.6 mg/kg by IV every 3 wks (n = 495) PD Capecitabine 1000 mg/m2 orally twice daily on Days 1-14, every 3 wks + Lapatinib 1250 mg/day orally continuously (n = 496) Primary endpoint: PFS by IRF, OS, safety Secondary endpoints: QoL (FACT B), DOR, PFS by investigator assessment Verma S, et al. NEJM 2012;367:1783-91. T-DM1 vs Lapatinib/Capecitabine in HER2+ MBC (EMILIA): PFS Median, Mos Proportion Progression Free 1.0 Capecitabine/lapatinib T-DM1 0.8 6.4 9.6 Events, n 304 265 Stratified HR: 0.650 (95% CI: 0.55-0.77; P < .0001) 0.6 0.4 T-DM1 Capecitabine/ lapatinib 0.2 0 0 2 4 6 8 10 12 14 16 18 20 22 24 26 28 30 Mos Verma S, et al. NEJM 2012;367:1783-91. Overall Survival – Second Interim Analysis Verma S, et al. NEJM 2012;367:1783-91. T-DM1 vs Lapatinib/Capecitabine in HER2+ MBC (EMILIA): Adverse Events T-DM1 (n = 490) Adverse Event, % Capecitabine + Lapatinib (n = 488) All Grades Grades ≥ 3 All Grades Grades ≥ 3 Diarrhea 23.3 1.6 79.7 20.7 Hand-foot syndrome 1.2 0 58.0 16.4 Vomiting 19.0 0.8 29.3 4.5 Hypokalemia 8.6 2.2 8.6 4.1 Fatigue 35.1 2.4 27.9 3.5 Nausea 39.2 0.8 44.7 2.5 Mucosal inflammation 6.7 0.2 19.1 2.3 Increased AST 22.4 4.3 9.4 0.8 Increased ALT 16.9 2.9 8.8 1.4 5.9 2.0 8.6 4.3 0 0 1.0 1.0 Anemia 10.4 2.7 8.0 1.6 Thrombocytopenia 28.0 12.8 2.5 0.2 Nonhematologic Hematologic Neutropenia Febrile neutropenia Verma S, et al. NEJM 2012;367:1783-91. T-DM1 vs Lapatinib/Capecitabine in HER2+ MBC (EMILIA): Expert Perspectives • T-DM1 showed improved efficacy vs capecitabine plus lapatinib – Significant PFS improvement (HR: 0.650; P < .0001) – OS benefit (HR: 0.68; P =<0.001) • Favorable safety profile • T-DM1 is an important new therapeutic option for patients with HER2+ MBC that has been previously treated with trastuzumab. Verma S, et al. NEJM 2012;367:1783-91. Ongoing Clinical Trials for Metastatic Breast Cancer Phase III MARIANNE Study: T-DM1 ± Pertuzumab in HER2+ MBC PD Trastuzumab + Taxane (n = 364) Patients with HER2+, previously untreated MBC T-DM1 + Pertuzumab (n = 364) (N = 1092) T-DM1 + Placebo (n = 364) • Primary endpoints: PFS as assessed by IRF, AEs – Superiority design with a noninferiority analyses – Interim futility analysis: option to drop experimental arm • Secondary endpoints: OS, TTF by IRF, ORR, CBR, DOR ClinicalTrials.gov. NCT01120184. mTOR Inhibition May Overcome Trastuzumab Resistance IGF-1R Nutrients Increased signaling through IGF-1R EGFR/HER2 Truncated HER2 PI3K PTEN Constitutive PI3K/AKT activation LKB1 AKT Absent or low PTEN AMPK TSC1 TSC2 Elevated AKT or pAKT RHEB Growth & proliferation Angiogenesis mTOR mTOR inhibitor Cell metabolism Widakowich C, et al. Anticancer Agents Med Chem. 2008;8:488-496. Miller TW, et al. Clin Cancer Res. 2009;15:7266-7276. Downstream inhibition with mTOR inhibitor counters these resistance mechanisms Synergy of mTOR inhibition and trastuzumab in vitro and in vivo BOLERO-1 Phase III Study: Paclitaxel + Trastuzumab Everolimus in HER2+ MBC Stratification by previous adjuvant or neoadjuvant trastuzumab and presence of visceral metastases Patients with HER2overexpressing, unresectable locally advanced or metastatic breast cancer, no previous trastuzumab or chemotherapy within 12 mos for advanced disease 28-day cycle 2:1 (N = 717) Everolimus 10 mg/day PO + Paclitaxel 80 mg/m2 on Days 1, 8, 15 + Trastuzumab 4 mg → 2 mg/kg on Days 1, 8, 15, 22 Paclitaxel 80 mg/m2 on Days 1, 8, 15 + Trastuzumab 4 mg → 2 mg/kg on Days 1, 8, 15, 22 + Placebo PO daily Primary endpoint: PFS Secondary endpoints: OS, ORR, CBR, safety, PK, biomarkers ClinicalTrials.gov. NCT00876395. Conclusions • Multiple effective and available options in HER2+ MBC – Trastuzumab – Pertuzumab – Lapatinib • Preferred first-line regimens include dual HER2 inhibition with pertuzumab and trastuzumab • Other HER2 inhibition agents continue to have a role outside the first-line setting including the new availability of TDM-1. Early Stage HER-2+ Breast Cancer Neo-Adjuvant Therapy GeparQuinto: HER2-Positive Doc Trastuzumab (T) R EC T for 6 mos Doc* Lapatinib (L) E: C: Doc: Surgery Core biopsy EC (d21-d35 after last infusion) (n=615) Epirubicin 90 mg/m² Cyclophosphamide 600 mg/m² Docetaxel 100mg/m² *+ G-CSF T for 12 mos T: Trastuzumab 6 (8) mg/kg L: 1000-1250 mg/d p.o. (all 3 week cycles) This presentation is the intellectual property of the author/presenter. Contact them for permission to reprint and/or distribute. Untch M, et al. Cancer Res. 2010;70(Nr. 24 Suppl):81s. Abstract # S3-1. pCR Rates According to Other Definitions No invasive residual in breast & nodes No invasive residual in breast P<0.05 This presentation is the intellectual property of the author/presenter. Contact them for permission to reprint and/or distribute. Untch M, et al. Cancer Res. 2010;70(Nr. 24 Suppl):81s. Abstract # S3-1. P<0.05 Neo-ALTTO Trial José Baselga, Ian Bradbury, Holger Eidtmann, Serena DiCosimo, Claudia Aura, Evandro de Azambuja, Henry Gomez, Phuong Dinh, Karine Fauria, Veerle Van Dooren, Paolo Paoletti, Aron Goldhirsch, Tsai-Wang Chang, Istvan Lang, Michael Untch, Richard D. Gelber and Martine Piccart-Gebhert on behalf of the Neo-ALTTO Study Team December 10, 2010 *FDA approved in combination with capecitabine, for the treatment of patients with advanced or metastatic breast cancer whose tumors overexpress HER2 and who have received prior therapy including an anthracycline, a taxane, and trastuzumab. Baselga J, et al. Cancer Res. 2010;70 (24 Suppl): Abstract S3-3. Study Design Baselga J, et al. Cancer Res. 2010;70 (24 Suppl): Abstract S3-3. Efficacy – pCR and to tpCR Baselga J, et al. Cancer Res. 2010;70 (24 Suppl): Abstract S3-3. pCR by Hormone Receptor Status Baselga J, et al. Cancer Res. 2010;70 (24 Suppl): Abstract S3-3. *Pertuzumab is not approved by the FDA for treatment of breast cancer. Gianni L, et al. Cancer Res. 2010;70 (24 Suppl): Abstract [S3-2]. NeoSphere Study Design and Objectives Gianni L, et al. Cancer Res. 2010;70 (24 Suppl): Abstract [S3-2]. NeoSphere pCR Rates: ITT Population Summary Gianni L, et al. Cancer Res. 2010;70 (24 Suppl): Abstract [S3-2]. NeoSphere: pCR and Hormone Receptors Status Gianni L, et al. Cancer Res. 2010;70 (24 Suppl): Abstract [S3-2]. NSABP B-41: Lapatinib in Neoadjuvant Treatment of HER2+ Breast Cancer Tissue biopsy for biomarker analysis Patients with HER2+, operable breast cancer (N = 529) Doxorubicin/Cyclophosphamide 60/600 mg/m2 q21d x 4 cycles → Weekly Paclitaxel 80 mg/m2 q28d x 4 cycles + Trastuzumab weekly until 1 wk before surgery (n = 178) Doxorubicin/Cyclophosphamide 60/600 mg/m2 q21d x 4 cycles → Weekly Paclitaxel 80 mg/m2 q28d x 4 cycles + Lapatinib 1250 mg/day until 1 day before surgery (n = 173) Tissue biopsy for biomarker analysis Surgery Trastuzumab 1 yr Doxorubicin/Cyclophosphamide 60/600 mg/m2 q21d x 4 cycles → Weekly Paclitaxel 80 mg/m2 q28d x 4 cycles + Trastuzumab weekly until 1 wk before surgery + Lapatinib 750 mg/day until 1 day before surgery (n = 173) • Primary endpoint: pCR Robidoux A, et al. ASCO 2012. Abstract LBA506. • Secondary endpoints: pCR in N0, toxicity, cCR, RFS, OS Lapatinib in Neoadjuvant Treatment of HER2+ Breast Cancer (NSABP B-41): pCR Regimen P Value† n pCR*, % AC → WP + T 176 49.4 AC → WP + L 171 47.4 .78 AC → WP + T + L 171 60.2 .056 *Absence of invasive tumor in resected breast specimen and histologically negative axillary nodes. †Relative to AC → WP + T regimen. Robidoux A, et al. ASCO 2012. Abstract LBA506. Adjuvant HER-2 Targeted Therapy NCCTG N9831 Trial Incorporating Trastuzumab in Adjuvant Therapy Group A HER2 positive (FISH+ or IHC 3+) n=3,505 R A N D O M I Z E AC T Group B AC T H Group C AC T H = AC (doxorubicin/cyclophosphamide 60/600 mg/m2 q3w × 4) = T (paclitaxel 80 mg/m2/wk × 12) = H (trastuzumab 4 mg/kg loading dose + 2 mg/kg/wk × 51) CP1270832-60 NSABP B-31 Trial Incorporating Trastuzumab in Adjuvant Therapy Group 1 Node positive HER2 positive (FISH+ or IHC 3+) N=2,006 R A N D O M I Z E AC T Group 2 AC T H = AC (doxorubicin/cyclophosphamide 60/600 mg/m2 q3w × 4) = T (paclitaxel 175 mg/m2 q3w × 4 or 80 mg/m2/wk × 12) = H (trastuzumab 4 mg/kg loading dose + 2 mg/kg/wk × 51) CP1270832-61 Joint Analysis of HER2+ Adjuvant Trials 2 Arms of N9831 + B-31 Control Group (n=1,979): AC T N9831 Group A AC B-31 Group 1 AC T T Trastuzumab Group (n=1,989): AC T+H N9831 Group C AC T H B-31 Group 2 AC T H = AC =T =T =H CP1270832-62 (doxorubicin/cyclophosphamide 60/600 mg/m2 q3w × 4) (paclitaxel 80 mg/m2/wk × 12) (paclitaxel 175 mg/m2 q3w × 4 or 80 mg/m2/wk × 12) (trastuzumab 4 mg/kg loading dose + 2 mg/kg/wk × 51) N9831 and NSABP B-31 Update Kaplan-Meier estimates of (A) event-free survival and (B) overall survival. P < .001 HR 0.52 P < .001 HR 0.61 ©2011 by American Society of Clinical Oncology Perez E A et al. JCO 2011;29:3366-3373 N9831 and NSABP B-31 Update Perez E A et al. JCO 2011;29:3366-3373 ©2011 by American Society of Clinical Oncology Events Per Year From Randomizaton Perez E A et al. JCO 2011;29:3366-3373 ©2011 by American Society of Clinical Oncology BCIRG 006 Update Breast Cancer International Research Group (BCIRG) 006 Trial: Treatment Schema HER2-positive tumor (FISH+); node-positive or high-risk node-negative disease S U R G E R Y R A N D O M I Z E AC T (n=1073) AC TH (n=1074) 52 weeks TCH (n=1075) 52 weeks Endpoints 1°: Disease-free survival (DFS) 2°: Overall survival, toxicity, pathologic and molecular markers = H = Trastuzumab 4 mg/kg loading dose = AC = doxorubicin/cyclophosphamide 60/600 mg/m2 q3w = H = Trastuzumab 2 mg/kg qw = T = docetaxel 100 mg/m2 q3w = H = Trastuzumab 6 mg/kg q3w = TC = docetaxel 75 mg/m2/carboplatin target AUC 6 mg/mL· min Radiation therapy and/or hormonal therapy may be given after completion of chemotherapy if indicated Slamon et al. 29th Annual San Antonio Breast Cancer Symposium, 2005; Herceptin ® (trastuzumab) PI. March 2009. 68 Disease-Free Survival Among all Study Patients DFS AC-TH vs AC-T HR .64 p<0.001 TCH vs AC-T HR .75 p=0.04 OS AC-TH vs AC-T HR .63 p<0.001 TCH vs AC-T HR .77 p=0.04 Overall OverallSurvival Survival DFS by Nodal Status at Randomization DFS by Nodal Status at Randomization Role of Anthracyclines? Controversies in Use of Anthracyclines • Authors suggest TCH should not be a preferred regimen for HER2+ early breast cancer. – BCIRG 006 not powered to show equivalence or non-inferiority between the two H-based regimens – Numerically fewer recurrences and deaths in the ACTH arm than TCH. Controversies in Use of Anthracyclines • Authors encourage use of anthracycline-based adjuvant trastuzumab regimens as a mainstay of therapy for women with higher-risk HER2+ tumors. • TCH should only be considered for women with lower-risk HER2+ tumors or in women with clinical reasons to avoid anthracyclines. Duration of Trastuzumab Pending Clinical Trials BETH Phase III Study: Chemotherapy + Trastuzumab ± Bevacizumab TCH HER2+, N+ or high-risk N- 6 x docetaxel and carboplatin RT (Group 1A) 1 yr of trastuzumab Stratified by Ns and HRS 6 x docetaxel and carboplatin (N ~ 3500) TCHB RT (Group 1B) 1 yr of trastuzumab Primary endpoint: IDFS Secondary endpoints: DFS, OS, RFI, DRFI, toxicity ClinicalTrials.gov. NCT00625898. 1 yr of bevacizumab ALTTO Trial Design Women with centrally determined HER2positive invasive breast cancer (N = 8381 accrued) Trastuzumab 8 mg/kg IV (loading dose)* 6 mg/kg every 3 wks for 1 yr Paclitaxel 80 mg/m2 IV once wkly x 12 Surgery, adjuvant anthracyclinebased therapy for 4 cycles; LVEF ≥ 50 *For concomitant dosing with paclitaxel, trastuzumab will be given on a weekly schedule (4 mg/kg IV loading dose followed by 2 mg/kg IV weekly). Trastuzumab will revert to the 3-weekly schedule (6 mg/kg without loading dose). 6-week wash-out Trastuzumab 4 mg/kg IV (loading dose) 2 mg/kg once wkly x 11 Paclitaxel 80 mg/m2 IV once wkly x 12 Lapatinib 1500 mg orally once daily x 34 wks Lapatinib 1500 mg/kg orally once daily x 51 wks Paclitaxel 80 mg/m2 IV once wkly x 12 (This arm closed in 9/2011 due to inferiority) Trastuzumab 8 mg/kg (loading dose) 6 mg/kg every 3 wks for 1 yr Lapatinib 1000 mg orally once daily x 51 wks Paclitaxel 80 mg/m2 IV once wkly x 12 APHINITY: Study Schema N = 3806 S U R G E R Y Central confirmation of HER2 status Randomization within 7 wks of surgery R A N D O M I Z A T I O N Start treatment within 1 wk ClinicalTrials.gov Identifier: NCT01358877 Chemotherapy + trastuzumab and pertuzumab Anthracycline or non-anthracycline–based chemotherapy allowed F O L L O W U P Chemotherapy + trastuzumab and placebo Anthracycline or non-anthracycline–based chemotherapy allowed Anti-HER2 therapy for a total of 1 yr (52 wks) Radiotherapy and/or endocrine therapy may be started at the end of adjuvant chemotherapy 10 Y R S Conclusions • Trastuzumab in addition to chemotherapy remains the standard for all “high-risk” HER-2+ early breast cancer. • Controversies exist regarding the following: – Use of anthracyclines – Definition of “high-risk” – Role of additional biologic agents to trastuzumab – Optimal duration of trastuzumab Final Thoughts • The addition of anti-HER2 therapy has changed the natural history of HER2+ early and metastatic breast cancer. • Combining different anti-HER2 agents in these settings also appears to have an improved outcome. • Pertuzumab and TDM-1 are newly approved for women with HER2+ metastatic breast cancer. • Their role in the adjuvant/neoadjuvant setting depends upon the maturation of current clinical trials.