Deletion of IKZF1 and Prognosis in Acute Lymphoblastic Leukemia

Overview

Journal N Engl J Med

Specialty General Medicine

Date 2009 Jan 9

PMID 19129520

Citations 628

Authors

Charles G Mullighan

Xiaoping Su

Jinghui Zhang

Ina Radtke

Letha A A Phillips

Christopher B Miller

Jing Ma

Wei Liu

Cheng Cheng

Brenda A Schulman

Richard C Harvey

I-Ming Chen

Robert J Clifford

William L Carroll

Gregory Reaman

W Paul Bowman

Meenakshi Devidas

Daniela S Gerhard

Wenjian Yang

Mary V Relling

Sheila A Shurtleff

Dario Campana

Michael J Borowitz

Ching-Hon Pui

Malcolm Smith

Stephen P Hunger

Cheryl L Willman

James R Downing

Affiliations

Soon will be listed here.

Abstract

Background: Despite best current therapy, up to 20% of pediatric patients with acute lymphoblastic leukemia (ALL) have a relapse. Recent genomewide analyses have identified a high frequency of DNA copy-number abnormalities in ALL, but the prognostic implications of these abnormalities have not been defined.

Methods: We studied a cohort of 221 children with high-risk B-cell-progenitor ALL with the use of single-nucleotide-polymorphism microarrays, transcriptional profiling, and resequencing of samples obtained at diagnosis. Children with known very-high-risk ALL subtypes (i.e., BCR-ABL1-positive ALL, hypodiploid ALL, and ALL in infants) were excluded from this cohort. A copy-number abnormality was identified as a predictor of poor outcome, and it was then tested in an independent validation cohort of 258 patients with B-cell-progenitor ALL.

Results: More than 50 recurring copy-number abnormalities were identified, most commonly involving genes that encode regulators of B-cell development (in 66.8% of patients in the original cohort); PAX5 was involved in 31.7% and IKZF1 in 28.6% of patients. Using copy-number abnormalities, we identified a predictor of poor outcome that was validated in the independent validation cohort. This predictor was strongly associated with alteration of IKZF1, a gene that encodes the lymphoid transcription factor IKAROS. The gene-expression signature of the group of patients with a poor outcome revealed increased expression of hematopoietic stem-cell genes and reduced expression of B-cell-lineage genes, and it was similar to the signature of BCR-ABL1-positive ALL, another high-risk subtype of ALL with a high frequency of IKZF1 deletion.

Conclusions: Genetic alteration of IKZF1 is associated with a very poor outcome in B-cell-progenitor ALL.

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