Whole Transcriptome Sequencing Reveals Recurrent NOTCH1 Mutations in Mantle Cell Lymphoma

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2012 Jan 3

PMID 22210878

Citations 144

Authors

Robert Kridel

Barbara Meissner

Sanja Rogic

Merrill Boyle

Adele Telenius

Bruce Woolcock

Jay Gunawardana

Catherine E Jenkins

Chris Cochrane

Susana Ben-Neriah

King Tan

Ryan D Morin

Stephen Opat

Laurie H Sehn

Joseph M Connors

Marco A Marra

Andrew P Weng

Christian Steidl

Randy D Gascoyne

Affiliations

Soon will be listed here.

Abstract

Mantle cell lymphoma (MCL), an aggressive subtype of non-Hodgkin lymphoma, is characterized by the hallmark translocation t(11;14)(q13;q32) and the resulting overexpression of cyclin D1 (CCND1). Our current knowledge of this disease encompasses frequent secondary cytogenetic aberrations and the recurrent mutation of a handful of genes, such as TP53, ATM, and CCND1. However, these findings insufficiently explain the biologic underpinnings of MCL. Here, we performed whole transcriptome sequencing on a discovery cohort of 18 primary tissue MCL samples and 2 cell lines. We found recurrent mutations in NOTCH1, a finding that we confirmed in an extension cohort of 108 clinical samples and 8 cell lines. In total, 12% of clinical samples and 20% of cell lines harbored somatic NOTCH1 coding sequence mutations that clustered in the PEST domain and predominantly consisted of truncating mutations or small frame-shifting indels. NOTCH1 mutations were associated with poor overall survival (P = .003). Furthermore, we showed that inhibition of the NOTCH pathway reduced proliferation and induced apoptosis in 2 MCL cell lines. In summary, we have identified recurrent NOTCH1 mutations that provide the preclinical rationale for therapeutic inhibition of the NOTCH pathway in a subset of patients with MCL.

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