Transcript Document
Clinical Dilemma: Which Adjuvant Chemotherapy is Just Right? Dr. Maureen Trudeau Head, Division of Medical Oncology/Hematology Toronto Sunnybrook Regional Cancer Centre Associate Professor, University of Toronto June 15, 2007 Systemic Therapy - Chemotherapy • Overall survival improvement in clinical trials both for standard and newer treatments • Choice – for patients, for physicians (anthracycline +/- taxanes) • Better decision making aids – www.adjuvantonline.com • Molecular profiles – Oncotype Dx, MammoPrint • Improved supportive care Decision Making in Adjuvant Therapy Tumour characteristics T, N, Grade, ER, PgR, Patient Characteristics HER2, LVI Age, Comorbidities Prior Therapy Performance Status Patient Preference Work/Family/Self Molecular Profile Clinical Trials, Guidelines Recent Reports Select Breast Cancer Treatments Based on Tumor Phenotype • Tumor phenotype defines treatment options Hormone receptor Positive Hormonal therapy Negative Chemotherapy HER2 HER2 Positive HER2-targeted therapy Negative Positive HER2-targeted therapy Negative IMPROVED RISK ASSESSMENT OF EARLY BREAST CANCER THROUGH GENE EXPRESSION PROFILING Gene-expression profile Good signature Poor signature microarray N Engl J Med, Vol 347 (25), Dec. 2002 March 2005 - Confidential BIGBIG-TRANSBIG Secretariat– Secretariat– Used with permission Breast Cancer is not ONE Disease Basal-like HER-2 “Normal” Luminal B Luminal A Sorlie T et al, PNAS 2001 Gene Expression Patterns of Breast Carcinomas ER Gene expression ER Gene expression O.S. A B C D E Basal-like HER2 Normal Luminal Luminal Subgroup Subgroup breast Subtype Subtype =E =D like C B Adapted from PNAS, 2001, vol 98 no. 19 Luminal Subtype A months ER+ 65-75% All Breast Cancer HER2+ 15-20% Basaloid 15% Molecular Classifications of Breast Tumors Luminal A ER + high Prolif - Luminal B + Basal -like ER + low ER - ERBB2 + Normal-like ER-/+ ER - -/+ - + P53 mutations 16% 71% 75%, also BRCA1 86% Sorlie 2007 The “Triple Negative” Breast Cancer Estrogen Receptor (ER) negative Progesterone receptor (PR) negative Her2neu (HER2) negative ER/PR/HER2 - Up to 90% of Triple Negative Breast Cancers are Basal-Like Breast Cancers Basal like Breast Cancers (BLC) • BLCs comprise 15% of all invasive cancers • More common in: – Younger pts – African Americans (40% premenopausal women) – BRCA1 mutation carriers • BLC are associated with: – high grade – p53 mutations – Increased expression of EGFR – CK5/6 (recent studies in 2006…Vimentin, cKIT, SRC) Sample • From the HBBC database, 1601 (80%) of patients had details on hormone receptors/HER2 and were eligible for the study • 180 (12%) of the 1601 patients were defined as basal-like breast cancers • Mean follow up was 8.1 years Characteristics of Basal-like versus Non basal-like Breast Cancers Characteristic Non Basal (N=1421) number (percent) Basal-like (N=180) number (percent) Significance p value * 57.7 53 p < 0.0001 2.1 cm 3.0 cm p < 0.0001 Mean Age at Diagnosis (yrs) Mean Tumor Size Tumor Size T1 (? 2 cm) T2 (>2cm to ? 5cm) T3 (>5cm) Missing 880 461 64 16 (62.7) (32.8) (4.6) 65 99 14 2 (36.5) (55.6) (7.9) p < 0.0001 Lymph Node Status Positive Negative Missing or Not Tested 510 609 302 (45.6) (54.4) 87 70 23 (54.4) (44.6) p = 0.02 237 616 336 (19.9) (51.8) (28.3) 15 37 101 (9.8) (24.2) (66.0) p < 0.0001 Tumor Grade I II III Missing * p values were calculated with the use of the chi-square test Hazard Rate of Distant Recurrence Survival Novel Therapies for TN • BRCA1 involved in repair of double stranded DNA breaks – Mutations implicated in breast/ovarian susceptibility • BRCA1 cancers appear to closely resemble sporadic triple negative breast cancers on molecular level • in vitro chemo-sensitivity studies have found that basal-like breast cancers may be particularly sensitive to cisplatin and to other drugs that cause double-strand breaks in DNA • Agents such as cisplatin and carboplatin may be more effective treatment than other types of chemotherapy for the basal like group Oncotype DX • A multigene assay to predict recurrence of Tamoxifen-treated, node-negative breast cancer (Paik NEJM 204) • 21 genes - proliferation (5), invasion (2), HER 2 (2), Estrogen (4) , 3 others and 5 reference genes with a Recurrence Score (RS) algorithm • For node negative, tam treated (JCO 2007): –Luminal A = low risk oncotype DX –Luminal B = mod/high risk Program for the Assessment of Clinical Cancer Tests (PACCT-1): Trial Assigning IndividuaLized Options for TReatment (TAILORx) TAILORx Participating Groups: ECOG, North American Breast Cancer Intergroup (CALBG, SWOG, NCCTG, NCIC, & ACOSOG) & NSABP Background: Management of ER-Positive, LymphNode Negative Breast Cancer • ~ 137,000 diagnosed annually in North America • ~ 80-85% are adequately treated with • surgery +/- irradiation • hormonal therapy • Adding chemotherapy recurrence by ~ 25% • absolute benefit is small (~3-5% or less) • Current practice guidelines • chemotherapy recommended for most Background: Practical Considerations for Selecting Oncotype DX Assay • Approved diagnostic test by regulatory agencies in the United States (CLIA) • No special processing required - may be performed on routinely collected and processed formalin-fixed, paraffin embedded tissue • Extensive post-marketing experience and familiarity in U.S. oncology community • Increasing precedent for third party reimbursement • Prior successful collaboration between NCIsponsored groups and industry partner Background: Scientific Rationale for Selecting Oncotype DX Assay 1. Validated prognostic test for tamoxifen treated patients – – – 2. predictive of distant recurrence may be used as dichotomous or continuous variable (Paik et al. NEJM, 2004) Also validated in population based Kaiser study – (Habel et al. SABCS 2004, abstr 3109) 3. Lower RS predictive of tamoxifen benefit – (Paik et al. ASCO 2005, abstr 510) 4. Higher RS predictive of chemotherapy benefit – (Paik et al. SABCS 2004, abstr 21) 5. Correlates more strongly with outcome than Adjuvant! – (Bryant et al. St. Gallen, 2005) 6. Predictive of local recurrence in tam treated patients – (Mamounas, SABCS 2005, abstr 29) Pre-REGISTER TAILORx Study Design ONCOTYPEDXASSAY REGISTER SpecimenBanking SecondaryStudy Group1 RS <11 ~29%of Population PrimaryStudyGroup RS11-25 ~44%of Population SecondaryStudy Group 2 RS>25 ~27%of Population ARMA Hormonal Therapy Alone RANDOMIZE StratificationFactors: Tumor Size, Menopausal Status, PlannedChemo, PlannedRadiation ARMD ChemotherapyPlus Hormonal Therapy ARMB ARMC Hormonal Therapy ChemotherapyPlus Alone Hormonal Therapy Background: Definition of Risk Groups for TAILORx • • • • Risk groups originally defined as (NEJM, 2004): – < 18 “Low Risk” – 18-30 “Intermediate Risk” – > 30 “High Risk” Definitions modified for TAILORx: – 11-25 “Primary Study Group” – < 11 “Secondary Study Group 1” – > 25 “Secondary Study Group 2” Rationale for selecting RS 11 as the lower bound for Primary Study Group: – RS predicts distant and local recurrence – RS 11: ~ 10% local & distant recurrence rate at 10 years – 10% threshold is typically used for recommending adjuvant chemotherapy Rationale for selecting 25 as upper bound for Primary Study Group: – RS 30 associated with 20% risk of distant recurrence – Lowering threshold to 25 reduces risk for undertreatment – When viewing chemotherapy and tamoxifen benefit as a continuous variables, 95% Confidence Intervals overlap in the 11-25 RS range (shown in next slides) Adapted by Dr. Maureen E. Trudeau, MD Anthracycline-based Regimens Superior To CMF/AC Regimen Trials Group DFS / OS (1) CEF (NCIC-CTG) (2) dd (EC) CEF (NCIC/EORTC/SAKK) -- -- (3) FEC100 > FEC50 (FASG) FEC50 CMF (ICCG) -- -- (4) CAF (SWOG) (5) E CMF (NEAT/SCTBG) (6) AV CF (MISSET) (7) TC (Jones) -- Taxane Regimens Superior To AC-type Regimens (1) (2) (3) (4) (5) (6) (1) (2) Regimen AC P AC P P FAC DAC FEC D A(C) D CMF Trials Group (CALGB) (NSABP) (MDACC) (BCIRG) (PACS 01) (BIG 2-98) Regimens superior to AC P dd AC P (CALGB) or dd A P C CEF or dd (EC) P DFS / OS --- - -- -- Adjuvant Chemotherapy Options – A Growing List 1998 CMF Options (F) AC (1970’s) (1980’s) 2007 Options CEF (CMF) FEC 100 (FEC 50) AC Taxol (AC) TAC (FAC) FEC 100 Docetaxel (FEC 100) Dose-dense AC Taxol (AC Taxol) Dose-dense (AC Taxol) (EC) Taxol CEF (AC Taxol) TAXANES AS ADJUVANT THERAPY SECOND GENERATION OF CLINICAL TRIALS Best taxane ECOG 1199 (intergroup trial) Dose & schedule Sequence vs combination Best taxane AC x 4 Px4 AC x 4 P weekly x 12 N5000 Taxane ± Herceptin® 2800 pts AC x 4 Dx4 AC x 4 D weekly x 12 Are There Factors that May Predict Response or Suggest which Therapy to Use? TAXANES AS ADJUVANT THERAPY SECOND GENERATION OF CLINICAL TRIALS Taxane ± Herceptin® Dose & schedule Sequence vs combination Best taxane Taxane ± Herceptin® N8700 • HERA: any chemo Herceptin: 0 vs 1 vs 2 yr • AC D vs AC D + H 1 yr vs DCH x 6 H 1 yr • AC P vs AC P + H 1 yr • AC P weekly x 12 vs AC P weekly x 12 H 1 yr vs AC P weekly x 12 + H 1 yr Trastuzumab DFS Median follow-up HERA 1 year Combined analysis 2 years DH 2 years BCIRG 006 DCarboH 2 years BCIRG 006 AC FinHER VH / DH 3 years CEF 0 Favors Trastuzumab 1 Favors no 2 Trastuzumab HR Piccart-Gebhart et al 2005; Romond et al 2005; Slamon et al 2005; Joensuu et al 2005 Average hazard reduction (Confidence interval) ER Neg DFS Pos Neg OS Pos 8541 LoHi 9344 Tax 9741 q3q2 Overall Loq2 36% 25% 23% 63% (15 to 52%) (11 to 36%) (0 to 42%) (43 to 76%) 14% 12% 10% 32% (-18 to 37%) (-4 to 25%) (-19 to 33%) (-7 to 56%) 29% 25% 22% 59% (3 to 48%) (11 to 37%) (-5 to 43%) (34 to 74%) 8% 10% 1% 18% (-27 to 36%) (-10 to 26%) (-44 to 32%) (-41 to 52%) Adjusted for pos nodes, T size, menopausal status Courtesy: Berry et al SABCS 2004 PACS 01 DFS by Age, ITT Age 50 yrs Age < 50 yrs 1.00 1.00 3FEC100-3D 0.75 0.75 Kaplan-Meier Estimate Kaplan-Meier Estimate 3FEC100-3D 6FEC100 0.50 Log-rank P-Value = 0.690 HR (Cox model) = 0.98 [0.77-1.25] 0.25 6FEC100 0.50 Log-rank P-Value = 0.001 HR (Cox model) = 0.67 [0.51-0.88] 0.25 Multivariate Interaction Test HR: 0.66 [0.46-0.95] P-value = 0.026 0.00 0 0.00 1 2 3 4 5 6 Survival Time (years) 7 8 0 1 2 3 4 5 Survival Time (years) 6 7 8 TAC vs FAC DFS by HER2 Status (Centrally reviewed, FISH centrally reviewed) % Alive and Disease-Free 100 Negative 90 100 Positive 90 80 TAC 80 TAC FAC 70 60 HR = 0.76 P = 0.046 50 70 60 HR = 0.60 P = 0.0088 FAC 50 0 6 12 18 24 30 36 42 48 54 60 66 0 6 12 18 24 30 36 42 48 54 60 66 Time to First Event Time to First Event Ratio of HRs 0.85 p= 0.4122 NEJM 2005 Topoisomerase II • Topoisomerase II is essential for DNA replication and recombination • Anthracyclines target topoisomerase II • Increased sensitivity to HER2 due to coamplification of TOP2A? A pooled analysis on the interaction between HER-2 expression and responsiveness of breast cancer to adjuvant chemotherapy Alessandra Gennari, Maria Pia Sormani, Matteo Puntoni and Paolo Bruzzi National Cancer Research Institute - Genoa and University of Genoa - Italy SABCS 2006 Characteristics of studies - I Study Comparison HER2 status determined (%) NSABP B11 PF vs PAF 638/682 (94%) NSABP B15 CMF vs AC 2.034/2.295 (89%) GUN 3 CMF vs CMF/EV 123/220 (56%) Brussels CMF vs HEC/EC 354/777 (46%) Milan CMF vs CMF→ A 506/552 (92%) DBCCG - 89 - D CMF vs FEC 805/980 (82%) NCIC MA5 CMF vs CEF 628/710 (88%) 5.088/6.216 (82%) Total (available/randomised) SABCS 2006 Disease Free Survival HER2 positive HER2 negative Study HR 95% CI NSABP B11 0.60 0.96 0.84 1.02 0.65 1.35 0.83 1.22 0.75 0.79 0.52 0.91 0.44 - 0.82 0.75 - 1.23 0.65 - 1.08 0.86 - 1.20 0.34 - 1.27 0.93 - 1.97 0.46 - 1.49 0.91 - 1.64 0.53 - 1.06 0.60 - 1.05 0.34 - 0.80 0.71 - 1.17 Total 0.90 0.82 - 0.98 p = 0.01 Overall 0.71 1.00 0.61 - 0.83 0.90 - 1.11 p < 0.0001 p = 1.0 NSABP B15 Brussels Milan DBCCG-89-D NCIC MA-5 heterogeneity 25 = 5.3, p = 0.38 heterogeneity 25 = 7.6, p = 0.18 anthra better 0.4 0.6 0.9 non anthra better 2 1 5 Test for interaction 2 = 13.7 p < 0.001 SABCS 2006 Efficacy summary HER2 positive • Risk of relapse HER2 negative • Risk of relapse 29% anthra ≈ non anthra HR 0.71 (0.61-0.83) HR 1.00 (0.90-1.11) (p < 0,0001) (p = 1,0) • Risk of death • Risk of death 27% anthra ≈ non anthra HR 0.73 (0.62-0.85) HR 1.03 (0.92-1.16) (p < 0,0001) (p < 0,86) SABCS 2006 Hierarchy of Chemotherapy Regimens Appropriate high risk population Older, no GCSF Younger, + GCSF Younger, +/- GCSF Younger, + GCSF Younger, + GCSF # of cycles 6 cycles 10 cycles 6 cycles (12 visits) 8 cycles 6 cycles High risk FECD dd(EC)P CEF dd(AC)P TAC FEC 100 CEF (MA 5) FEC 50 CMF is better than Moderate risk CAF ACP AC P AC D AC DC AD is better than Low Risk P = paclitaxel D = docetaxel No Therapy FAC The choice of chemotherapy Depends on the following: • Tumour characteristics and risk of relapse • Patient comorbidities • Patient age • Social determinants • Drug availability / costs • Physician or patient preference Cost of common regimens Regimen N+ Study Total Treatment Costs USD (drug acquisition + incidental + administration) DAC AC ->P AC->P CE120F FE100C FE100C->D BCIRG001 CALGB9344 CALGB9741 MA-5 FASG-5 PACS-01 $8,226 $4,340 $11,741 $4,852 $3,557 ~ $6,200 Convenience of common regimens Regimen N+ Study TAC BCIRG001 AC ->T CALGB9344 AC->T CALGB9741 CE120F MA-5 FE100C FASG-5 FE100C->D PACS-01 Visits 6 8 8 12 6 6 Chair time (h) 14 21.6 21.6 5.4 9 8 Where are we going? Adapted by Dr. Maureen E. Trudeau, MD Cases A 68-year old woman presents with an infiltrating duct carcinoma • 1.2 cm in size • ER 80% PR 60% • HER 2 • Sentinel node negative A 68-year old woman presents with an invasive ductal carcinoma A 59-year old postmenopausal woman with invasive ductal carcinoma • 1.9 cm in size • ER 30% PR 0% • HER 2+ (3+ by IHC) • Grade 3 • Sentinel node negative A 59-year old postmenopausal women with invasive ductal carcinoma A 49-year old premenopausal woman with invasive lobular carcinoma • 2.5 cm in size • ER 70% PR 30% • HER 2• Grade 2 • 2/10 positive lymph nodes A 49-year old premenopausal woman with invasive lobular carcinoma A 39-year old premenopausal woman with invasive ductal carcinoma • 2.8 cm in size • ER 0% PR 0% • HER 2 • Grade 3 • 5 nodes positive A 44-year old premenopausal woman with invasive ductal carcinoma • 2.0 cm in size • ER 100% PR 100% • HER 2 • Grade 2 • 1/17 nodes positive • 2 other smaller lesions, grade 1