2013 SABCS Review

1. 2013 SABCS Review Shou-Ching Tang MD, PhD, FACP, FRCP (C) GRU Cancer Center

2. Disclosure Nothing to declare

3. outline • Prognostic and predictive biomarkers • Prevention • Early breast cancer • locally advanced breast cancer • Advanced breast cancer • Targeted therapy • Conclusion

4. Prognostic and predictive biomarkers

5. Genetic landscape of MBCBachelot et al, #S6-07, SABCS 2013 • Exome sequencing of 100 pairs of MBC and normal breast tissue DNA (Integragen Inc, Hiseq platform) • Targeted sequencing of 100 genes in 240 MBC biopsies • PIK3CA 26%, AKT1 4%, PTEN 4%, ERBB 2%, K-Ras 1%, ATM 1%, CDH1 2%, GATA3 2%. PTPN11 1%, PTPRD 1%, ROS1 1% • Many of them are drugable and involved in metastatic process and drug resistance

6. Exome sequencing to identify actionable mutations in mTNBCBlackwell et al, S4-04, SABCS 2013 • 38 pts with mTNBC and matched specimens of germ-line DNA, primary and metastatic tumors • Whole-exome sequencing by Agilent solution-based system of exon capture with 10 GB of sequencing data • Striking genetic heterogeneity between primary and metastatic tumors continues

7. Exome sequencing to identify actionable mutations in mTNBCBlackwell et al, S4-04, SABCS 2013 • No single driver mutation that was common to metastatic tumors, indicating diverse genetic pathways contributing to metastasis • Mutations in APC and mTOR more frequent in metastatic than primary tumors • Nonsense mutations of ER in primary and metastatic tumors but not in germ-line DNA • EGFR and HER2 mutations not detected

8. Gene mutations and protein expression in TNBC vs non-TNBCO’Shaughnessy et al, #PD4-1, SABCS 2013 • 5500 pts evaluated for mutation (Sanger or IlluminaTruseq), protein expression (IHC) and/or amplification/rearrangement (FISH or CISH), 16% with TNBC • Mutation: TNBC has higher p53 mutation (60% vs 30%), lower PIK3CA (12% vs 31%) • Amplification: TNBC has higher amplification of EGFR (24% vs 13%), lower HER2, PIK3CA, cMYC and TOP2A • IHC: TNBC has higher AR (56% vs 15%)

9. Community-based NGS to guide clinical trial selectionYardley et al, abst PD4-3, SABCS 2013 • 594 advanced BC profiled • Most frequently altered gene: PIK3CA (24%), followed by RUNX1 (4%) and FGFR3 (2%) • Infrequent: PIK3R1, MET, KRAS, KIT, FGFR2, HER2, BRAF, SMO, MYC, DDR2 and AKT1, one pt each • 6% pts enrolled in phas I trials based on NGS (PI3K and mTOR inhibitor), 29% pts potentially eligible for ongoing trials at SCRI • PIK3CA mutation accounted for 70% of 35% actionable mutations detected

10. PI3KCA mutation predicts resistance in HER2+/ER+ BCLoibl et al, #S4-06, SABCS 2013 • Prospectively analyzed 512 pts from Geparsixto and validated in 225 pts from GeparQuinto trials • PI3KCA mutation found in 19.2% HER2+ tumors, more in HER2+/ER+, 21.5% pCR in pts with and without PI3KCA mutation 22.7 vs 43.6 %, p=0.001 with HER2+/ER+ tumors 6.5% vs 30.8%, p=0.005 No difference in HER2+/ER- tumors 42.9% vs 46.1%, p=0.852

11. PIK3CA mutation and/or low PTEN predict resistance to lapatinib and trastuzumabContreras, et al, #PD1-2, SABCS 2013 • Neoadjuvant L plus T (no chemo) x 12 wks • 59 pts tested for PTEN (IHC) and 33 for PI3KCA mutation (36% by NGS) • pCR: overall 16% high vs low PTEN 32% vs 9% p=0.04 PIK3CA mutation: 0% p=0.06 low PTEN and PIK3CA mutation vs normal: 0% vs 36% p=0.01

12. Prognostic value of tumor infiltrating lymphocytes (TIL’s) • % of lymphocyte infiltration in tumor stroma reflects host immune reaction • The presence of TIL’s was correlated with benefit from: • trastuzumab in HER2+ EBC in 156 pts from the neoadjuvant GeparQuattro trial (Loi et al, #S1-05, SABCS 2013) • the addition of carbo to neoadjuvant therapy in TN and HER2+ EBC in Geparsixto trial (Dunkert, et al, #S1-06) • adjuvant therapy in ECOG 2197 and 1199 in TNBC (Adams et al, #S1-07, SABCS 2013)

13. SWOG S0500 CTC’s in guiding CT in MBCSmerage et al, #S5-07, SABCS 2013 (CTC found in 75% MBC, half >5CTC/7.5 ml whole blood) Primary end point: OS

18. SWOG S0500 CTC’s in guiding CT in MBCSmerage et al, #S5-07, SABCS 2013 • Conclusion: • CTC prognostic in MBC at baseline and after first chemo • Changing chemo based on CTC after first chemo does not affect OS or PFS

19. prevention

20. IBIS-II Chemo-prevention in high risk postmenopausal womenCuzick et al, #S3-01, SABCS 2013 • Randomized phase III UK trial • 3864 women with high risks of BC, median f/u 5.03 yrs • Primary end point: incidence of BC, including DCIS • Anastrozole vs placebo for 5 years

21. IBIS-II: Chemo-prevention in high risk postmenopausal womenCuzick et al, #S3-01, SABCS 2013 • 5-yr BC incidence: 53% reduction, p<0.0001 • Significant reduction in all invasive BC (50%), ER+ BC (58%) and DCIS (70%) • Significant reduction of cancer at other sites (RR=0.58) • Deaths from BC and other causes similar in both arms • Musculoskeletal and vosomotor events higher and bone # non-significantly higher in anastrozole arm • In support of other chemoprevention trials: TAM (NSABP P-1), raloxifen (STAR)and exemestane (MAP3)

22. Early breast cancer

23. Hormone and physical exercise (HOPE) in EBCIrwin et al, #S3-03, SABCS 2013 • Randomized phase III multicenter US trial • 121 pts on adjuvant AI for > 6 m and with >3/10 worst joint pain on Brief Pain Inventory-Short form (BPI) • 150 min/wk mod-intense aerobic exercise and twice-wkly supervised resistance exercise or usual care • Primary end point: change in BPI worse joint pain score between 0-12 momths • reduction of BPI score (20% vs 3% , p=0.017), joint pain intensity (p=0.025), body wt (p=0.0057) and increase in cardiopulmonary fitness (p=0.024) • Impact on adherence to AI’s and survival?

24. Bisphosphonates and survival in EBC: meta-analysisColeman et al, #S4-07, SABCS 2013 36 randomized trials, 22,982 pts Primary end point: time to recurrence, to first distance recurrence and breast cancer mortality

25. Bisphosphonates and survival in EBC: meta-analysisColeman et al, #S4-07, SABCS 2013 RR 10-yr gain % 2p value All pts BC mortality 0.91 1.7 0.04 distance recurrence 0.92 1.3 0.05 Post-menopausal pts BC mortality 0.83 3.1 0.004 distance recurrence 0.83 3.3 0.0007

26. Bisphosphonates and survival in EBC: meta-analysisColeman et al, #S4-07, SABCS 2013 • Reduction in bone relapse in postmenopausal pts similar regardless of type of BP tx, duration and schedule or concomitant chemotherapy • Adjuvant BP improves survival in postmenopausal pts with EBC • No benefit in premenpausalpts in bone or other recurrences • Currently indicated for prevention or treatment of bone loss

27. Phase II study of TH in HER2+ and node- EBCTolaney, S et al, #S1-04, SABCS 2013 • 410 pts, HER2+ EBC • T1mi 3%; T1a 27%, T1b 20%, T1C 41%, T2<3 cm 9% • Wkly paclitaxel x12 with trastusumab for one year • Null hypothesis: 3-year failure rate of 9.2% (failure) • Alternative hypothesis: 3-year failure rate of 5% (success) • Due to limited number of events, DMSB approved data release with 1316 PYFU and median f/u of 3.2 years

29. TH in node-/HER2+ EBC • TH is highly effective and well tolerated • Can be considered an option in majority of stage 1 HER2+ EBC • Single arm study, 67% HR+ tumor, limited follow up of 3.6 years • Superior survival data suggest not all pts with stage 1 HER2+ EBC require trastuzumab-based chemotherapy, esp those with T1aN0 tumor • Addition of another biological agent to TH backbone is unlikely to have substantial benefit in this pt population (TDM-1 vs TH ongoing)

30. Primary results of BETH trial in HER2+, node+ or node- high risk EBCSlamon D et al, #S1-03, SABCS 2013 3509 pts, phase III Median f/u 3 years Invasive disease-free survival (IDFS) BETH Trial Docetaxel x 6 Carboplatin x 6 Trastuzumab x 1 y Bevacizumab 15mg q3 wk x 1 y 92% or 5-FU x 3 Epirubicin x 3 Cylophos x 3 Docetaxel x 3 Trastuzumab x 1 y Observation 8%

35. BETH primary result • Addition of one year bevacizumab to chemotherapy did not prolong invasive disease-free survival (IDFS) • TCH is an effective adjuvant regimen for pts with HER2+ EBC, including node+ tumors • No new or unexpected safely signals • No added benefit of bev in MBC, LABC and EBC in unselected pts, biomarker studies urgently needed (ongoing repeat of ECOG trial with biomarkers included)

36. GIM-2 EC or FEC with dd P or not in node+ EBCCognetti et al, # S5-06, SABCS 2013 • Italian multicenter randomized phase III 2x2 design • 2019 pts, node+, < 70 yo, median f/u 7 yrs • EC x4 or FEC x4 then P q 2 (with G) or 3 wks x4 • Primary end point: DFS • DD CT improved DFS and OS : HR 0.78 (p=0.007) and 0.68 (p=0.002) respectively • Benefit of DD CT independent of HR status • Addition of F to EC did not improve outcome

37. PRIME II: Adjuvant RT in pts > 65 yoKunkler et al, #S2-01, 2013 SABCS • Multicenter UK trial, 1326 pts, median f/u 5 yrs • >65 yo, T 1-2 (up to 3 cm), N0/M0, HR+, margin > 1mm, could be grade 3 or LVI but not both, required adjuvant hormonal therapy • Primary end point: ipsilateral breast tumor recurrence no RT(%) RT (%) p • IBTR 4.1 1.3 0.01 • OS 93.8 94.2 0.24 • Regional relapse 1.4 0.5 • Contralateral relapse 0.9 1.9 • Distance relapse 1.0 0.3 • Results similar to CALGB, ECOG and RTOG trial (pASCO 2010) • Omission of adjuvant RT safe in selected older pts

38. 10-yr survival update of NSABP B-32Julian et al, #S2-05, SABCS 2013 • Randomized phase III of SLND plus ALND or ALND • 5611 pts • Still no difference in OS, DFS and loco-regional relapse (HR 1.09, p=0.35; HR 1.02, p=0.72; HR 0.96, p=0.77 respectively) • No difference in OS and DFS in pts with occult mets detected by IHC with or without ALND • IHC has no prognostic role in EBC

39. Locally advanced breast cancer

40. Neo ALTTO Survival updatePiccar-Gebhart, M et al, #S1-01, SABCS 2013 Invasive operable HER2+ BC T > 2 cm (inflammatory BC excluded) LVEF  50% N=450 lapatinib lapatinib paclitaxel R A N D O M I Z E S U R GE R Y F E C X 3 trastuzumab trastuzumab paclitaxel • Stratification: • T ≤ 5 cm vs. T > 5 cm • ER or PgR + vs. • ER & PgR – • N 0-1 vs. N ≥ 2 • Conservative surgery • or not lapatinib lapatinib trastuzumab trastuzumab paclitaxel 6 wks + 12 wks 34 weeks Median f/u 3.77 years 52 weeks of anti-HER2 therapy

41. NeoALTTO Efficacy – pCR and tpCR L: lapatinib; T: trastuzumab; L+T: lapatinib plus trastuzumab pCR pathologic complete response HR: hormone receptors Baselga J et al. SABCS 2010; abstract S3-3

46. NeoALTTO survival update • First study to show that pts with pCR had significantly better EFS and OS with HER2+ tumors • Study was powered to detect difference in pCR, but underpowered to detect moderate difference in survival • Dual HER2 blockade is superior • HER2+/HR- and HER2+/HR+ subgroups are different diseases

47. TRIO-US B07 final analysisHurvitz S et al, #S1-02, SABCS 2013 • Randomized phase II of neoadjuvant H or L or both in stage 1-3, HER2+ EBC • 106 pts in 13 US centers, primary end point, pCR • Run-in cycle of H or L or both followed by 6 cycles of TCH (A) vs TCL (B) or TCHL (C) • OveralpCR: 42% (A 43%, B 25% and C 52%, p=0.069) • Pair-wise comparison: pCR in B significantly lower than C (p=0.021), not different between A and B (p=0.14) and A and C (p=0.45)

48. CALGB 40603 (Alliance) neoadjuvant carbo +/- Bev in TNBCSikov et al, #S5-01, SABCS 2013 2x2 randomized phase II in locally advanced TNBC in 545 pts

49. CALGB 40603 (Alliance) neoadjuvantcarbo +/- Bev in TNBCSikov et al, #S5-01, SABCS 2013 • pCR (%, breast and axilla): no CbCb Bev effect No Bev 28.2 42.4 10.5 Bev 42.6 50.0 p=0.031 Cb benefit 10.3 p=0.033 • Addition of Cb or Bev to NAC significantly increases pCR in TNBC, and the increases are additive • Several studies now support the addition of Cb to standard CT in LABC (CALGB 40604, GeparSixto and I-Spy 2), adjuvant trials ongoing

50. I-SPY 2 TRIAL: Learn, Drop, Graduate, and Replace Agents Over Time Paclitaxel+ Trastuzumab Key Paclitaxel + Trastuzumab* + New Agent A Randomize MRI AC HER 2 (+) Surgery Paclitaxel + Trastuzumab* + New Agent B Residual Disease (Pathology) Learn and adapt from each patient as we go along Paclitaxel + Trastuzumab* + New Agent F Paclitaxel + Trastuzumab* + New Agent C Patient is on Study Paclitaxel Randomize Paclitaxel + New Agent F Paclitaxel + New Agent C AC HER 2 (–) Surgery Paclitaxel + New Agent GH Paclitaxel + New Agent D Paclitaxel + New Agent E *Investigational agent may be used in place