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Slamon D et al. SABCS 2009;Abstract 62.

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Presentation on theme: "Slamon D et al. SABCS 2009;Abstract 62."— Presentation transcript:

1 Slamon D et al. SABCS 2009;Abstract 62.
BCIRG 006 Phase III Trial Comparing AC  T with AC  TH and with TCH in the Adjuvant Treatment of HER2-Amplified Early Breast Cancer Patients: Third Planned Efficacy Analysis Slamon D et al. SABCS 2009;Abstract 62.

2 Introduction Trastuzumab treatment is associated with cardiac dysfunction, especially in patients who have received anthracyclines. Pre-clinical data suggested that there is a synergy between trastuzumab and docetaxel/carboplatin that is not seen with anthracyclines. Current study objectives: Assess the efficacy, safety and cardiac safety of an anthracycline regimen compared to the same regimen with trastuzumab (H) versus a nonanthracycline regimen with H in patients with HER2-amplified early breast cancer. Source: Slamon D et al. SABCS 2009;Abstract 62.

3 R BCIRG 006: Study Design Eligibility HER2+ by central FISH
Accrual: 3,222 (Closed) Eligibility HER2+ by central FISH Node positive or high risk node negative Stratified by nodes and hormone receptor status AC  T R AC  TH TCH AC  T = AC (Adriamycin 60 mg/m2, Cyclophosphamide 600 mg/m2) q 3 weeks x 4 followed by T (Docetaxel 100 mg/m2) q 3 weeks x 4 AC  TH = AC (Adriamycin 60 mg/m2, Cyclophosphamide 600 mg/m2) q 3 weeks x 4 followed by T 100 mg/m2 q 3 weeks x 4. Trastuzumab (H) initiated with T x 1 year TCH = T (75 mg/m2) and Carboplatin (AUC 6) q 3 weeks x 6. H initiated with TC x 1 year Source: Slamon D et al. SABCS 2009;Abstract 62.

4 BCIRG 006: Tumor Characteristics
n = 1073 % AC  TH n = 1074 TCH n = 1075 Number of Nodes (+) 1-3 4-10 > 10 29 38 22 11 24 9 39 23 10 Tumor Size (cm) ≤ 2 > 2 and ≤ 5 > 5 41 53 6 55 7 40 54 ER and/or PR (+) Source: Slamon D et al. SABCS 2009;Abstract 62.

5 Disease Free Survival (DFS) 3rd Planned Analysis (median follow-up 65 mos)
1 0.9 84% 0.8 81% 75% 0.7 % alive and disease-free 0.6 Patients Events HR (95% C.I.) P (reference) ( ) <0.001 ( ) AC-T AC-TH 0.5 TCH 0.4 12 24 36 48 60 72 Time (months) Source: With permission Slamon D et al. SABCS 2009;Abstract 62.

6 Overall Survival 3rd Planned Analysis (median follow-up 65 mos)
1 92% 0.9 91% 87% 0.8 0.7 % alive 0.6 Patients Events HR (95% C.I.) P (reference) ( ) <0.001 ( ) AC-T AC-TH 0.5 TCH 0.4 12 24 36 48 60 72 Time (months) Source: With permission Slamon D et al. SABCS 2009;Abstract 62.

7 DFS According to Nodal and Topo IIa Amplification Status
Lymph Node Status AC  T AC  TH TCH Lymph node negative (n=309, 310, 309) 85% 93% 90% Lymph node positive (n=764, 764, 766) 71% 80% 78% Lymph nodes ≥ 4 (n=350, 350, 352) 61% 73% 72% Topo IIa Amplification Topo IIa non co-amplified (n=643, 643, 618) 70% 83% Topo IIa co-amplified (n=328, 357, 359) 82% Source: Slamon D et al. SABCS 2009;Abstract 62.

8 Safety Endpoints No cardiac related deaths were observed in any of the three study arms. Grade 3/4 CHF was lower in the TCH arm. 0.4% with TCH versus 0.7% with AC  T versus 2% with AC  TH. The incidence of >10% decline in LVEF was lower in the TCH arm. 9% with TCH versus 19% with AC  TH versus 11% with AC  T Eight patients in BCIRG 006 have developed acute leukemias to date. Six cases in AC  T, one case in AC  TH and one case in TCH (patient received CHOP for subsequent diagnosis of lymphoma prior to acute leukemia development) Source: Slamon D et al. SABCS 2009;Abstract 62.

9 BCIRG 006: Therapeutic Index
AC  TH n = 1074 TCH n = 1075 DFS Events 185 214 Grade 3 / 4 CHF 21 4 Totals 206 218 Treatment-related leukemias 1 1* Sustained LVEF loss > 10% 194 97 * Leukemia developed after CHOP chemotherapy Source: Slamon D et al. SABCS 2009;Abstract 62.

10 Conclusions: BCIRG 006 Trastuzumab provides a similar and significant advantage for both DFS and OS in low- and high-risk patients when used either as AC  TH or as TCH. Acute and chronic toxicity profiles of TCH are better than AC  TH. Though there is no statistical advantage, the AC  TH arm had a 29 event numerical advantage in DFS events over that of the TCH arm. Numerical advantage, however, was associated with 5 times more cases of CHF in the AC  TH arm than in the TCH arm. All three regimens showed similar efficacy in a subset of patients with Topo IIa co-amplification. The incremental benefit of AC that is known for HER2+ BC appears restricted to TOPO IIa co-amplified cancers. Source: Slamon D et al. SABCS 2009;Abstract 62.

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