Rituximab Improves the Efficacy of High-dose Chemotherapy with Autograft for High-risk Follicular and Diffuse Large B-cell Lymphoma: a Multicenter Gruppo Italiano Terapie Innnovative Nei Linfomi Survey

Overview

Journal J Clin Oncol

Specialty Oncology

Date 2008 May 21

PMID 18490650

Citations 22

Authors

Corrado Tarella

Manuela Zanni

Michele Magni

Fabio Benedetti

Caterina Patti

Tiziano Barbui

Alessandro Pileri

Mario Boccadoro

Fabio Ciceri

Andrea Gallamini

Sergio Cortelazzo

Ignazio Majolino

Salvo Mirto

Paolo Corradini

Roberto Passera

Giovanni Pizzolo

Alessandro M Gianni

Alessandro Rambaldi

Affiliations

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Abstract

Purpose: To investigate the impact of adding rituximab to intensive chemotherapy with peripheral-blood progenitor cell (PBPC) autograft for high-risk diffuse large B-cell lymphoma (DLB-CL) and follicular lymphoma (FL).

Patients And Methods: Data were collected from 10 centers associated with Gruppo Italiano Terapie Innnovative nei Linfomi for 522 patients with DLB-CL and 223 patients with FL (median age, 47 years) who received the original or a modified high-dose sequential (HDS) chemotherapy regimen. HDS was delivered to 396 patients without (R-) and to 349 patients with (R+) rituximab; 154 (39%) and 178 patients (51%) in the R- and R+ subsets, respectively, underwent HDS for relapsed/refractory disease.

Results: A total of 355 R- (90%) and 309 R+ patients (88%) completed the final PBPC autograft. Early treatment-related mortality was 3.3% for R- and 2.8% for R+ (P = not significant). Two parameters significantly influenced the outcome: disease status at HDS, with 5-year overall survival (OS) projections of 69% versus 57% for diagnosis versus refractory/relapsed status, respectively, and rituximab addition, with 5-year OS of 69% versus 60% in the R+ versus R- groups, respectively. In the multivariate analysis, these two variables maintained an independent prognostic value. The marked benefit of rituximab was evident in patients receiving HDS as salvage treatment: the 5-year OS projections for R+ versus R- were, respectively, 64% versus 38%, for patients with refractory disease or early relapse and 71% versus 57%, for patients with late relapse, partial response, or second/third relapse.

Conclusion: The results of this large series indicate that rituximab should be included in the current practice of PBPC autograft for DLB-CL and FL.

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