Eastern cooperative oncology group E1496: ECOG and CALGB Cyclophosphamide/Fludarabine (CF) with or without Maintenance Rituximab (MR) in Advanced Indolent.

Slides:

Advertisements

Similar presentations

Palumbo A et al. Proc ASH 2013;Abstract 536.

Advertisements

An Intergroup Randomised Trial of Rituximab versus a Watch & Wait Approach in Patients with Advanced Stage, Asymptomatic, Non-bulky Follicular Lymphoma.

Follicular lymphoma Optimal primary therapy and consolidation ? Seminars in Hematological Oncology * Israel, April M. Dreyling, Dept. of Medicine.

1 N9841: A Randomized Phase III Equivalence Trial of Irinotecan (CPT-11) versus FOLFOX4 in Patients with Advanced Colorectal Carcinoma Previously Treated.

Supervisor: Vs 楊慕華醫師 Presenter: CR 周益聖醫師 N Engl J Med 2012;367:

Casulo C et al. Proc ASH 2013;Abstract 510.

Spotlight on Chronic Lymphocytic Leukemia and Indolent Non-Hodgkin's Lymphoma: European and US Perspectives on the Evolving Standard of Care Bruce Cheson,

Presented by Martin H. Cohen, M.D. at the 27 July 2004 meeting of the Oncologic Drugs Advisory Committee.

Jonathan W. Friedberg M.D., M.M.Sc. University of Rochester Medical Center Optimal frontline therapy for Follicular lymphoma: Do we need to start with.

Rituximab Maintenance: Stage III/IV Follicular Lymphoma (ECOG/CALGB E1496) Subset: 237 FL pts CVP x 6-8 → PR/CR (cyclophosphamide, vincristine, prednisone)

Phase III Study Comparing Gemcitabine plus Cetuximab versus Gemcitabine in Patients with Locally Advanced or Metastatic Pancreatic Adenocarcinoma Southwest.

HELIOS – Klinikum Erfurt

Intergroup trial CALGB 80101

Alliance/CALGB 50803: A Phase 2 Trial of Lenalidomide plus Rituximab in Patients with Previously Untreated Follicular Lymphoma1 The ‘RELEVANCE’ Trial:

1 SNDA Gemzar plus Carboplatin Treatment of Late Relapsing Ovarian Cancer.

Results of Docetaxel Plus Oxaliplatin (DOCOX) +/- Cetuximab in Patients with Metastatic Gastric and/or Gastroesophageal Junction Adenocarcinoma: Results.

NHL13: A Multicenter, Randomized Phase III Study of Rituximab as Maintenance Treatment versus Observation Alone in Patients with Aggressive B ‐ Cell Lymphoma.

Consolidation treatment with Y 90 Ibritumomab Tiuxetan after R-CHOP induction in high-risk patients with Follicular Lymphoma (FL) (GOTEL-FL1LC): a multicentric,

Phase III trial of chemotherapy with or without irinotecan in the front-line treatment of metastatic colorectal cancer in elderly patients. FFCD

Alternating Courses of CHOP and DHAP Plus Rituximab (R) Followed by a High-Dose Cytarabine Regimen and ASCT is Superior to Six Courses of CHOP Plus R Followed.

Randomized Phase III Trial Comparing FOLFIRINOX (F: 5FU/Leucovorin [LV], Irinotecan [I], and Oxaliplatin [O]) versus Gemcitabine (G) as First-Line Treatment.

Rituximab maintenance for the treatment of indolent NHL Dr Christian Buske.

E2100 A Randomized Phase III Trial of Paclitaxel versus Paclitaxel plus Bevacizumab as First- Line Therapy for Locally Recurrent or Metastatic Breast Cancer.

Dyer MJS et al. Proc ASH 2014;Abstract 1743.

A phase III trial comparing R-CHOP 14 and R-CHOP 21 for the treatment of newly diagnosed diffuse large B cell lymphoma Results from a UK NCRI Lymphoma.

Bortezomib (VELCADE), Rituximab, Cyclophosphamide, Dexamethasone (VRCD) combination therapy in front-line low-grade non-Hodgkin lymphoma (LG-NHL) is active.

Head-to-Head Comparison of Obinutuzumab (GA101) plus Chlorambucil (Clb) versus Rituximab plus Clb in Patients with Chronic Lymphocytic Leukemia (CLL) and.

Rituximab Maintenance versus Wait and Watch After Four Courses of R-DHAP Followed by Autologous Stem Cell Transplantation in Previously Untreated Young.

A Phase 3 Study Evaluating the Efficacy and Safety of Lenalidomide Combined with Melphalan and Prednisone Followed by Continuous Lenalidomide Maintenance.

Rituximab plus Lenalidomide Improves the Complete Remission Rate in Comparison with Rituximab Monotherapy in Untreated Follicular Lymphoma Patients in.

Optimal use of rituximab in aggressive NHL

1 Flinn I et al. Proc ICML 2013;Abstract 084.

Frontline Chemoimmunotherapy with Fludarabine (F), Cyclophosphamide (C), and Rituximab (R) (FCR) Shows Superior Efficacy in Comparison to Bendamustine.

Phase II trial of irinotecan/docetaxel for advanced pancreatic cancer with randomization between irinotecan/docetaxel and irinotecan/docetaxel plus C225,

Safety and Efficacy of Abbreviated Induction with Oral Fludarabine (F) and Cyclophosphamide (C) Combined with Dose-Dense IV Rituximab (R) in Previously.

Gemcitabine With or Without Cisplatin in Patients with Advanced or Metastatic Biliary Tract Cancer (ABC): Results of a Multicentre, Randomized Phase III.

What is the best approach for a follicular lymphoma patient who achieves CR after frontline chemoimmunotherapy? Radioimmunotherapy! Matthew Matasar,

Low Dose Decitabine Versus Best Supportive Care in Elderly Patients with Intermediate or High Risk MDS Not Eligible for Intensive Chemotherapy: Final Results.

An Open-Label, Randomized Study of Bendamustine and Rituximab (BR) Compared with Rituximab, Cyclophosphamide, Vincristine, and Prednisone (R-CVP) or Rituximab,

Chemoimmunotherapy with Fludarabine (F), Cyclophosphamide (C), and Rituximab (R) (FCR) versus Bendamustine and Rituximab (BR) in Previously Untreated and.

Phase II Trial of R-CHOP plus Bortezomib Induction Therapy Followed by Bortezomib Maintenance for Previously Untreated Mantle Cell Lymphoma: SWOG 0601.

Journal Club Dr. Eyad Al-Saeed Radiation Oncology 12 January, 2008.

Rituximab Maintenance After Chemoimmunotherapy Induction in 1 st and 2 nd Line Improves Progression Free Survival: Planned Interim Analysis of the International.

Nabhan C et al. Proc ICML 2013;Abstract 102.

Brentuximab Vedotin in Combination with RCHOP as Front-Line Therapy in Patients with DLBCL: Interim Results from a Phase 2 Study Yasenchak CA et al. Proc.

Mok TS, Wu SL, Thongprasert S, et al. Gefitinib or carboplatin-paclitaxel in pulmonary adenocarcinoma. N Engl J Med. 2009;361: Gefitinib Superior.

Single-agent nab-Paclitaxel Given Weekly (3/4) as First-line Therapy for Metastatic Breast Cancer (An International Oncology Network Study, #I )

Treatment of non-Hodgkin Lymphomas

GALLIUM: Obinutuzumab- vs Rituximab-Based Immunochemotherapy in Patients With Untreated Follicular Lymphoma New Findings in Hematology: Independent Conference.

Summary Author: Dr. C. Tom Kouroukis, MD MSc FRCPC

Geisler C et al. Proc ASH 2011;Abstract 290.

A Phase III Randomized Intergroup Trial (SWOG S0016) of CHOP Chemotherapy plus Rituximab vs CHOP Chemotherapy plus Iodine-131-Tositumomab for the Treatment.

Alessandra Gennari, MD PhD

NCI 9177: Risk-Adapted DA-EPOCH-R in Adults With Burkitt Lymphoma

Attal M et al. Proc ASH 2010;Abstract 310.

CREATE-X: Adjuvant Capecitabine in HER2-Negative Breast Cancer

ASSIST-FL: Rituximab Biosimilar GP2013 vs Rituximab in Treatment-Naive Patients With Advanced Follicular Lymphoma New Findings in Hematology: Independent.

CALGB/Alliance 50303: R-CHOP vs DA-EPOCH-R in Newly Diagnosed Diffuse Large B-Cell Lymphoma New Findings in Hematology: Independent Conference Coverage.

Kahl BS et al. Proc ASH 2011;Abstract LBA-6.

Fowler NH et al. Proc ASCO 2010;Abstract 8036.

Jonathan W. Friedberg M.D., M.M.Sc.

Coiffier B et al. Proc ASH 2010;Abstract 857.

CTCL: INNOVATIVE TREATMENTS GEMCITABINE

Vitolo U et al. Proc ASH 2011;Abstract 777.

What is the optimal management of an asymptomatic 62 year old with low tumor burden, stage IV, grade 1-2 FL? Answer: R-chemotherapy Peter Martin,

Michael E. Williams, MD, ScM

What is the optimal management of a 43-year-old man with high-risk FL not in CR after R-chemo? Answer: Radioimmunotherapy Peter Martin, M.D. The Charles,

Faderl S et al. Proc ASCO 2011;Abstract 6503.

What is the best frontline regimen for CLL patients

The Argument Why This Patient SHOULD Receive “Maintenance” Rituximab

Presentation transcript:

eastern cooperative oncology group E1496: ECOG and CALGB Cyclophosphamide/Fludarabine (CF) with or without Maintenance Rituximab (MR) in Advanced Indolent Lymphoma Patients: Results from the E1496 Trial Howard S. Hochster Edie Weller Randy D. Gascoyne Theresa S. Ryan Thomas M. Habermann Leo I. Gordon Stanley R. Frankel Sandra J. Horning

eastern cooperative oncology group E1496: Rationale and Objectives  Indolent Lymphoma – responsive to chemotherapy with long survival  Therapy is rarely curative with continuous relapse pattern  Hypothesis: Chemotherapy induction to maximal benefit followed by therapy with anti-CD20 antibody will improve progression free survival  To compare the response rate, PFS, and OS for treatment with CF (cyclophosphamide ‑ fludarabine) to a control arm consisting of standard treatment with CVP  To determine the effect of maintenance with anti ‑ CD20 (rituximab) on time to progression, time to treatment failure, and survival for CF and CVP  Indolent Lymphoma – responsive to chemotherapy with long survival  Therapy is rarely curative with continuous relapse pattern  Hypothesis: Chemotherapy induction to maximal benefit followed by therapy with anti-CD20 antibody will improve progression free survival  To compare the response rate, PFS, and OS for treatment with CF (cyclophosphamide ‑ fludarabine) to a control arm consisting of standard treatment with CVP  To determine the effect of maintenance with anti ‑ CD20 (rituximab) on time to progression, time to treatment failure, and survival for CF and CVP

eastern cooperative oncology group E1496 Study History  Accrual 3/98 - 2/00  Suspended with 115 CF and 119 CVP R patients  32 CF deaths vs 8 CVP deaths (ASCO 2001)  Reopened 11/00: CVP induction (CVP T ) +/- maintenance rituximab  Terminated at 2nd interim analysis Prolonged PFS with MR (ASCO 2004)  This Analysis  Examine Effect of maintenance rituximab on CF and randomized CVP (CVP R ) patients

eastern cooperative oncology group E1496 Eligibility  Stage III-IV  Low-grade (WF) histology: A,B,C  Untreated, measurable disease  Age > 18 years, ECOG 0-1  Adequate organ function  Prospective assessment of tumor burden  Stage III-IV  Low-grade (WF) histology: A,B,C  Untreated, measurable disease  Age > 18 years, ECOG 0-1  Adequate organ function  Prospective assessment of tumor burden

eastern cooperative oncology group E 1496 Study Design CF Cyclophosphamide 1000 mg/m 2 IV d 1, Fludarabine 20 mg/m 2 iv d 1-5 Repeat q 28 d; best response + 2 cycles (6- 8) MRRituximab 375 mg/m2 wkly x 4 Start 4 wk after chemotherapy, every 6 m for 2 yr CF Cyclophosphamide 1000 mg/m 2 IV d 1, Fludarabine 20 mg/m 2 iv d 1-5 Repeat q 28 d; best response + 2 cycles (6- 8) MRRituximab 375 mg/m2 wkly x 4 Start 4 wk after chemotherapy, every 6 m for 2 yr Observation MR CVPn=119 CF(n=115) RANDOMIZERANDOMIZE RANDOMIZERANDOMIZE RESTAGERESTAGE Advanced Indolent NHL CR, PR, SD Stratify: Histology, age, Tumor burden Stratify: Histology, Residual Disease* CF CF(n=69) CVPn=95 *Minimal residual disease = 75% reduction in large mass

eastern cooperative oncology group E1496 Study Treatment (revised) C Cyclophosphamide 1000 mg/m 2 IV d 1 V Vincristine 1.4 mg /m 2 (max = 2) IV d 1 P Prednisone 100 mg/m 2 PO d 1-5 Repeat q 21 d; best response + 2 cycles (6- 8) MR Rituximab 375 mg/m 2 wkly x 4 Start 4 wk after CVP; every 6 m for 2 y Observation (OBS) Maintenance Rituximab (MR) CVP RANDOMIZERANDOMIZE RESTAGERESTAGE CR, PR, SD Stratify: Histology, Residual disease N=282

eastern cooperative oncology group E1496 Study Population CFCVP R CVP CVP T Total Patients Path exclusion Other Ineligible Eligible Maintenance Randomization Eligible and randomized67*89*304 * All path exclusions

eastern cooperative oncology group E1496 Induction Patient Characteristics (%) CF (n = 110) CVP R (n =112) CVP CVP T(n=379) Age > Median age (years) Male Follicular histology Stage IV PS High tumor burden LDH elevated B symptoms present Bone marrow involved737970

eastern cooperative oncology group E1496 Induction Toxicity (%) Grade 3-5 toxicity CF(n=115) CVP R (n =119) CVP T (n =401) p value Neutropenia82% 37% 37%30%< Thrombopenia29%4%3%< Febrile neutropenia 3%0%1%0.12 Infection17%5%7%0.003 Pulmonary7%3%3%0.25 N, V 10%2%2%0.01

eastern cooperative oncology group E1496 Grade 5 Toxicity (n) TOXICITYCF(n=115) CVP R (n=119) p value Infection/sepsis Liver20NS CNS10NS Cardiac01NS MAINTENANCE Infection4*00.03 *1 = OBS; 3 MR

eastern cooperative oncology group E1496: Response to Induction chemotherapy CF (n=110) CVP R (n=112) p value p value CR 56 (51%) 25 (22%) < PR 38 (35%) 61 (55%) NS SD 5 (5%) 16 (14%) NS RR 94 (86%) 77 (77%) NS

eastern cooperative oncology group E1496 Maintenance Randomization Reason Reason CF (n=46) CVP R (n=24) p value p value Central pathology review 3 (6%) 2 (8%) 0.66 Progressive disease 11 (24%) 11 (46%) 0.10 Induction toxicity 19 (41%) 1 (4%) Pt refusal or withdrawal 6 (13%) 4 (17%) 0.73 Other/unknown 7 (15%) 6 (25%) 0.22 Induction Patients Not Proceeding to 2nd Randomization

eastern cooperative oncology group E1496 Maintenance Patient Characteristics (%) CF(n=67) CVP R CVP R(n=89) MR (n = 34) OBS (n =33) MR (n = 48) OBS (n =41) Age > Median age (years) Male Follicular histology Stage IV PS High tumor burden LDH elevated B symptoms present Bone marrow involved Minimal Residual Disease (p<0.0001)

eastern cooperative oncology group E1496 Maintenance Toxicity (%) CF(n=69) CVP R (n=95) Grade 3-5 toxicity MR (n = 35) OBS (n =34) MR (n = 49) OBS (n =46) Neutropenia Thrombopenia Febrile neutropenia 3000 Infection Pulmonary12300 Diarrhea9300

eastern cooperative oncology group E1496: Response to Maintenance Therapy CF(n=67) CVP R (n=89) p-value p-value CR 41 (61%) 24 (27%) PR 22 (33%) 53 (60%) SD 3 (5%) 11 (12%) 0.10 RR 63 (94%) 9 (87%) 0.18 Improved Response after randomization 9/25 (36%) 20/64 (31%) 0.81

eastern cooperative oncology group Progression Free Survival CF vs CVP Patients Median 3.8 vs. 3.3 y Logrank p=0.19 HR=0.8 (0.6,1.1)

eastern cooperative oncology group Overall Survival CF vs CVP Patients Years from Induction Randomization CF (110) CVP (112)

eastern cooperative oncology group Progression Free Survival MR vs OBS for Induction CVP Years from Maintenance Randomization Probability Median 4.9 vs. 1.3 y Logrank p=0.004 HR=0.5 (0.3,0.8) MR (48) OBS (41)

eastern cooperative oncology group Progression Free Survival MR vs OBS for Induction CF Years from Maintenance Probability Median NR vs. 5.0 y Logrank p=0.19 HR=0.7 (0.4,1.5) MR (34) OBS (33)

eastern cooperative oncology group Progression Free Survival CF vs. CVP +/- maintenance rituximab Years from Maintenance Randomization Probability CF-MR (34) CF-OBS (33) CVP-MR (48) CVP-OBS (41)

eastern cooperative oncology group Overall Survival MR vs OBS for Induction CVP Years from Maintenance Randomization Probability MR (48) OBS (41) Median NR vs. NR Logrank p=0.21 HR = 0.7 (0.3,1.6)

eastern cooperative oncology group Overall Survival MR vs OBS for Induction CF Years from Maintenance Randomization Probability MR (34) OBS (33) Median NR vs. NR Logrank p=0.42 HR = 1.1 (0.4,2.9)

eastern cooperative oncology group Overall Survival CF vs. CVP +/- maintenance rituximab Years from Maintenance Randomization Probability CF-MR (34) CF-OBS (33) CVP-MR (48) CVP-OBS (41)

eastern cooperative oncology group E1496: CONCLUSIONS   Induction CF (E1496 dose & schedule), compared to CVP, resulted in:   Higher CR and OR rates (56 vs 25%; 94 vs 77%)   Higher minimal disease rates (95 vs 65%)   Increased induction toxicity and mortality (gr 3-5 hematologic toxicity = 96 vs 59% )   Maintenance rituximab after induction:   Was given to fewer CF patients due to induction toxicity   Was associated with greater toxicity after CF.   Prolonged PFS after CVP but not after CF.   Induction CF (E1496 dose & schedule), compared to CVP, resulted in:   Higher CR and OR rates (56 vs 25%; 94 vs 77%)   Higher minimal disease rates (95 vs 65%)   Increased induction toxicity and mortality (gr 3-5 hematologic toxicity = 96 vs 59% )   Maintenance rituximab after induction:   Was given to fewer CF patients due to induction toxicity   Was associated with greater toxicity after CF.   Prolonged PFS after CVP but not after CF.

eastern cooperative oncology group E1496: CONCLUSIONS   CF followed by observation resulted in longer PFS (median 5 y) than the CVP-observation arm (median 1.3 y, p= 0.02)   Similar to CVP-MR arm (median 4.9 yrs)   No differences in OS observed to date.   CF in E1496 dose and schedule cannot be recommended due to toxicity.   Results suggest that a more effective induction regimen can translate into longer PFS and that the benefit of MR may be more difficult to demonstrate in that setting.   CF followed by observation resulted in longer PFS (median 5 y) than the CVP-observation arm (median 1.3 y, p= 0.02)   Similar to CVP-MR arm (median 4.9 yrs)   No differences in OS observed to date.   CF in E1496 dose and schedule cannot be recommended due to toxicity.   Results suggest that a more effective induction regimen can translate into longer PFS and that the benefit of MR may be more difficult to demonstrate in that setting.

eastern cooperative oncology group With our Thanks:  Co-investigators  Institutional investigators  Data Management staff  ECOG Operations Office and Statistical Center staffs  Patients  Co-investigators  Institutional investigators  Data Management staff  ECOG Operations Office and Statistical Center staffs  Patients