Integrated Mutational and Cytogenetic Analysis Identifies New Prognostic Subgroups in Chronic Lymphocytic Leukemia

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2012 Dec 18

PMID 23243274

Citations 197

Authors

Davide Rossi

Silvia Rasi

Valeria Spina

Alessio Bruscaggin

Sara Monti

Carmela Ciardullo

Clara Deambrogi

Hossein Khiabanian

Roberto Serra

Francesco Bertoni

Francesco Forconi

Luca Laurenti

Roberto Marasca

Michele Dal-Bo

Francesca Maria Rossi

Pietro Bulian

Josep Nomdedeu

Giovanni Del Poeta

Valter Gattei

Laura Pasqualucci

Raul Rabadan

Robin Foa

Riccardo Dalla-Favera

Gianluca Gaidano

Affiliations

Soon will be listed here.

Abstract

The identification of new genetic lesions in chronic lymphocytic leukemia (CLL) prompts a comprehensive and dynamic prognostic algorithm including gene mutations and chromosomal abnormalities and their changes during clonal evolution. By integrating mutational and cytogenetic analysis in 1274 CLL samples and using both a training-validation and a time-dependent design, 4 CLL subgroups were hierarchically classified: (1) high-risk, harboring TP53 and/or BIRC3 abnormalities (10-year survival: 29%); (2) intermediate-risk, harboring NOTCH1 and/or SF3B1 mutations and/or del11q22-q23 (10-year survival: 37%); (3) low-risk, harboring +12 or a normal genetics (10-year survival: 57%); and (4) very low-risk, harboring del13q14 only, whose 10-year survival (69.3%) did not significantly differ from a matched general population. This integrated mutational and cytogenetic model independently predicted survival, improved CLL prognostication accuracy compared with FISH karyotype (P < .0001), and was externally validated in an independent CLL cohort. Clonal evolution from lower to higher risk implicated the emergence of NOTCH1, SF3B1, and BIRC3 abnormalities in addition to TP53 and 11q22-q23 lesions. By taking into account clonal evolution through time-dependent analysis, the genetic model maintained its prognostic relevance at any time from diagnosis. These findings may have relevant implications for the design of clinical trials aimed at assessing the use of mutational profiling to inform therapeutic decisions.

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