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Il Paziente senza target

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Presentation on theme: "Il Paziente senza target"— Presentation transcript:

1 Il Paziente senza target
Grande Lung Slam Roma, 9 Ottobre 2015 Il Paziente senza target Francesco Grossi U.O.S. Tumori Polmonari IRCCS Azienda Ospedaliera Universitaria San Martino IST Istituto Nazionale per la Ricerca sul Cancro Genova

2 Interlinking factors to guide personalized therapy in caucasian NSCLC patients
80% of patients Clinical Factors Histologic Factors Molecular Factors 20% of patients

3 ASCO practice guideline update (1/2)
Masters GA, JCO 2015

4 ASCO practice guideline update (2/2)
Masters GA, JCO 2015

5 Old algorithm for the therapy of advanced NSCLC
Proposed treatment algorithm EGFR mutation positive or ALK fusion positive Molecular Good PS Clinical (PS) Poor PS EGFR TKIs or Crizotinib Nonsquamous Histologic Squamous Single-agent chemotherapy Bevacizumab eligible First line Clinical Bevacizumab ineligible Platinum/pemetrexed (or other*) ± bevacizumab Platinum/pemetrexed (or other*) Platinum/gemcitabine (or other*) End of first-line chemotherapy Maintenance Bevacizumab or erlotinib or pemetrexed Pemetrexed or erlotinib Erlotinib Based on prior therapy Progression Second line Chemotherapy by algorithm Based on prior therapy Based on prior therapy Based on prior therapy *Docetaxel, paclitaxel, or vinorelbine. Adapted from Gandara DR, Clin Lung Cancer 2009

6 Biomarker-unselected non-squamous NSCLC in the real life
Present/Future algorithms: Cisplatin + Pemetrexed  Pemetrexed (maintenance)  Docetaxel + Nintedanib/Erlotinib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line) Carboplatin + Paclitaxel + Bevacizumab  Bevacizumab (maintenance)  Pemetrexed/ Erlotinib/Docetaxel+Nintedanib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line)

7 Biomarker-unselected squamous NSCLC in the real life
Present/Future algorithm: Cisplatin + Gem/VNR/Taxanes  Nivolumab/ Docetaxel/Erlotinib (IInd line) Erlotinib/Nivolumab (IIIrd line)  Erlotinib/Nivolumab (IVth line)

8 Biomarker-unselected non-squamous NSCLC in the real life
Present/Future algorithms: Cisplatin + Pemetrexed  Pemetrexed (maintenance)  Docetaxel + Nintedanib/Erlotinib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line) Carboplatin + Paclitaxel + Bevacizumab  Bevacizumab (maintenance)  Pemetrexed/ Erlotinib/Docetaxel+Nintedanib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line)

9 JMDB: OS in non-squamous & squamous patients
Scagliotti G, JCO 2008

10 Continuation maintenance:
Continuation (PARAMOUNT) or switch (JMEN) maintenance with pemetrexed: OS Continuation maintenance: PARAMOUNT Switch maintenance: JMEN 13.9 mos vs 11.0 mos (+2.9mos) 16.9 mos vs 14 mos (+2.9mos) 13.4 mos vs 10.6 mos (+2.8mos) 16.5 mos vs 13.9 mos (+2.6mos)

11 Association between TS and efficacy of pemetrexed: PFS & OS
Wang T, PLOS ONE 2013

12 A better clinical outcome with pemetrexed/cisplatin in low TS only
Sun JM, J Clin Oncol 2015

13 E4599: Bevacizumab-based therapy until progression increases OS
Sandler A, JTO 2010 & NEJM 2006

14 Efficacy of first-line regimens: pre-planned OS & PFS analyses in adenocarcinoma patients
1. Scagliotti G, Oncologist Sandler A, JTO 2010

15 PRONOUNCE: Study Design
Randomized, open-label, phase III superiority study conducted in US Pemetrexed 500 mg/m2, Carboplatin AUC 6 (Pem+Cb) Paclitaxel 200 mg/m2, Carboplatin AUC 6, Bevacizumab 15 mg/kg (Pac+Cb+Bev) Induction Phase q21d, 4 cycles Maintenance Phase q21d until PD Bev-Eligible Population Inclusion: - Chemo-naïve patients - PS 0/1 - Stage IV, nonsquam - Stable treated CNS mets Exclusion: - Uncontrolled effusions Pemetrexed (folic acid & vitamin B12) + Carboplatin Pemetrexed (folic acid & vitamin B12) R 1:1 180 patients each Paclitaxel + Carboplatin + Bevacizumab Bevacizumab Stratified for: PS (0 vs 1); gender (M vs F); disease stage (M1a vs M1b) Zinner RG, JTO 2015 15

16 PRONOUNCE Zinner RG, JTO 2015

17 PointBreak: study design
Randomized, open-label, phase III superiority study conducted in US Pemetrexed 500 mg/m2; Carboplatin AUC 6; Bevacizumab 15 mg/kg Paclitaxel 200 mg/m2; Carboplatin AUC 6; Bevacizumab 15 mg/kg Induction Phase q21d, 4 cycles Maintenance Phase q21d until PD Inclusion: - No prior systemic therapy for lung cancer - PS 0/1 - Stage IIIB-IV NS-NSCLC - Stable tx’t brain mets Exclusion: Peripheral neuropathy > Gr 1 - Uncontrolled pleural effusions Pemetrexed (folic acid & vitamin B12 ) + Carboplatin + Bevacizumab Pemetrexed (folic acid & vitamin B12 ) + Bevacizumab R 1:1 450 patients each Paclitaxel + Carboplatin + Bevacizumab Bevacizumab Stratified for: PS (0 vs 1); sex (M vs F); disease stage (IIIB vs IV); measurable vs nonmeasurable disease Patel JD, JCO 2013 17

18 PointBreak: PFS and OS from randomization (ITT)
Patel JD, JCO 2013

19 Primary endpoint Overall Survival
ECOG 5508: Schema Bevacizumab IIIB/IV NSCLC PS0/1 No Prior Tx N=1495 R A N D M I Z E Carboplatin Paclitaxel Bevacizumab X 4 cycles CR PR SD N=897 Pemetrexed Bevacizumab Pemetrexed Stratification Factors: Smoking status, Gender Histology, Best response, Stage Primary endpoint Overall Survival Status: Accrual completed April 2015

20 AvaALL: bevacizumab continued beyond progression in NSCLC
Primary endpoint: OS Stage IIIB/IV non-squamous NSCLC treated with platinum- doublet (4–6 cycles) + bevacizumab PLUS > 2 cycles of bevacizumab maintenance SOC2* + bevacizumab SOC3‡ + bevacizumab SOC4 ± bevacizumab Randomise 1:1 PD1 PD2 PD3 SOC2* SOC3‡ SOC4 Enroll n=600 Graphical elaboration from text data Primary endpoint: OS Secondary endpoints include PFS, safety, QoL and biomarker analysis *SOC2: labelled agents for second-line treatment of NSCLC ‡SOC3 and beyond: choice of labelled agents is the investigator’s choice Gridelli C, Clin Lung Cancer 2011

21 Trials with PD-1 Inhibitors Added to E4599 Backbone
Arm 1 - Control Carbo/Paclitaxel + Bevacizumab Untreated Non-squamous Stage IV NSCLC Arm 2 Carbo/Paclitaxel + Bevacizumab + PD-1 Inhibitor Atezolizumab: carbo/paclitaxel +/- bevacizumab +/- atezolizumab N=1200, PFS primary endpoint Identifier: NCT Pembrolizumab: Keynote-021- phase I-II, PFS, N=308, One arm is Pembro/carbo/paclitaxel/ bevacizumab Identifier: NCT Additional trial looks at bevacizumab maintenance with nivolumab (Identifier:NCT )

22 Second-line strategies in EGFR w/t or ALK- patients
Old second-line Docetaxel Pemetrexed Erlotinib New second-line Nivolumab Docetaxel+nintedanib

23 Biomarker-unselected non-squamous NSCLC in the real life
Present/Future algorithms: Cisplatin + Pemetrexed  Pemetrexed (maintenance)  Docetaxel + Nintedanib/Erlotinib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line) Carboplatin + Paclitaxel + Bevacizumab  Bevacizumab (maintenance)  Pemetrexed/ Erlotinib/Docetaxel+Nintedanib/Nivolumab (IInd line)  Erlotinib/Nivolumab (IIIrd line)  Erlotinib/ Nivolumab (IVth line)

24 Docetaxel vs Docetaxel+Nintedanib (LUME Lung 1): PFS and OS
Adenocarcinoma & time since start of first-line therapy of less than 9 months Total population Adenocarcinoma Adenocarcinoma Total population Squamous-cell Reck M, Lancet Oncol 2014

25 Docetaxel vs Docetaxel+Nintedanib (LUME Lung 1): toxicities
Reck M, Lancet Oncol 2014

26 BeTa: Erlotinib ± Bevacizumab in the second-line setting
Erlotinib 150mg/day + Bevacizumab 15mg/kg every 3 weeks PD Previously treated advanced non-squamous NSCLC Erlotinib 150mg/day orally + placebo PD Arm N RR (%) Median PFS (mos) Median OS (mos) Erlotinib 6.2 1.7 9.2 Beva+Erlot 12.6 3.4 9.3 HR 0.62 0.97 P-value 0.006 <0.0001 0.75 Herbst RS, Lancet 2011

27 Adenocarcinoma: second-line treatment options

28 CheckMate 057 (NCT01673867) Study Design
Randomize 1:1 Stage IIIB/IV non-SQ NSCLC Pre-treatment (archival or recent) tumor samples required for PD-L1 ECOG PS 0–1 Failed 1 prior platinum doublet Prior maintenance therapy alloweda Prior TKI therapy allowed for known ALK translocation or EGFR mutation N = 582 Nivolumab 3 mg/kg IV Q2W until PD or unacceptable toxicity n = 292 Docetaxel 75 mg/m2 IV Q3W until PD or unacceptable toxicity n = 290 Primary Endpoint OS Additional Endpoints ORRb PFSb Safety Efficacy by tumor PD-L1 expression Quality of life (LCSS) Patients stratified by prior maintenance therapy and line of therapy (second- vs third-line) PD-L1 expression measured using the Dako/BMS automated IHC assay14,15 Fully validated with analytical performance having met all pre-determined acceptance criteria for sensitivity, specificity, precision, and robustness a Maintenance therapy included pemetrexed, bevacizumab, or erlotinib (not considered a separate line of therapy); b Per RECIST v1.1 criteria as determined by the investigator. Paz-Ares L , ASCO 2015

29 CheckMate 057: OS update Horn L , ECCO/ESMO 2015

30 Biomarker-unselected squamous NSCLC in the real life
Present/Future algorithm: Cisplatin + Gem/VNR/Taxanes  Nivolumab/ Docetaxel/Erlotinib (IInd line) Erlotinib/Nivolumab (IIIrd line)  Erlotinib/Nivolumab (IVth line)

31 Squire: study design Thatcher N, ASCO 2014

32 Squire: primary outcome OS
Thatcher N, Lancet Oncol2015

33 Nab-Paclitaxel vs paclitaxel: study design and objectives
Stage IIIb/IV NSCLC No prior therapy for metastatic disease ECOG PS 0-1 N = 1052 sb-Paclitaxel 200 mg/m2 d1 (3-h infusion) Carboplatin AUC 6 d1 21-day cycles with premedication of dexamethasone + antihistamines nab®-Paclitaxel 100 mg/m2 d1, 8, 15 (30-min infusion) No premedication Stratification factors: Stage (IIIb vs IV); age; (< 70 vs ≥ 70); sex; histology (adenocarcinoma vs squamous cell vs other); geographic region Objective: To compare the efficacy and safety of nab-paclitaxel plus carboplatin vs sb-paclitaxel plus carboplatin in advanced NSCLC Primary endpoint: ORR by independent radiological review (CR + PR) Secondary endpoints: PFS, OS, DCR (CR + PR + SD), and safety Socinski MA, JCO 2012

34 Nab-Paclitaxel vs paclitaxel: PFS and OS
Socinski MA, JCO 2012 Socinski MA et al. J Clin Oncol April 30. [Epub ahead of print].

35 Biomarker-unselected squamous NSCLC in the real life
Present/Future algorithm: Cisplatin + Gem/VNR/Taxanes  Nivolumab/ Docetaxel/Erlotinib (IInd line) Erlotinib/Nivolumab (IIIrd line)  Erlotinib/Nivolumab (IVth line)

36 CheckMate 017 (NCT01642004) - Study Design
Nivolumab 3 mg/kg IV Q2W until PD or unacceptable toxicity n = 135 Docetaxel 75 mg/m2 IV Q3W until PD or unacceptable toxicity n = 137 Randomize 1:1 Primary Endpoint: OS Additional Endpoints: Investigator-assessed ORR Investigator-assessed PFS Correlation between PD-L1 expression and efficacy Safety Quality of life (LCSS) Stage IIIb/IV SQ NSCLC 1 prior platinum doublet- based chemotherapy ECOG PS 0–1 Pre-treatment (archival or fresh) tumor samples required for PD-L1 analysis N = 272 Patients stratified by region and prior paclitaxel use One pre-planned interim analysis for OS At time of DBL (December 15, 2014), 199 deaths were reported (86% of deaths required for final analysis) The boundary for declaring superiority for OS at the pre-planned interim analysis was P <0.03 Spigel DR , ASCO 2015

37 CheckMate 017: OS update Reck M , ECCO/ESMO 2015

38 Docetaxel vs Docetaxel + Ramucirumab (Revel trial): OS and PFS
Garon EB, Lancet Oncology 2014

39 Docetaxel vs Docetaxel + Ramucirumab (Revel trial): toxicities
Garon E, Lancet 2014

40 NSCLC: “old” schedules and OS
Pemetrexed/Bevacizumab/Histology 8 Reck M, Lancet 2013

41 Grazie per l’attenzione!

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