Precision and Prognostic Value of Clone-specific Minimal Residual Disease in Acute Myeloid Leukemia

Overview

Journal Haematologica

Specialty Hematology

Date 2017 Mar 18

PMID 28302711

Citations 24

Authors

Pierre Hirsch

Ruoping Tang

Nassera Abermil

Pascale Flandrin

Hannah Moatti

Fabrizia Favale

Ludovic Suner

Florence Lorre

Christophe Marzac

Fanny Fava

Anne-Claire Mamez

Simona Lapusan

Francoise Isnard

Mohamad Mohty

Ollivier Legrand

Luc Douay

Chrystele Bilhou-Nabera

Francois Delhommeau

Affiliations

Soon will be listed here.

Abstract

The genetic landscape of adult acute myeloid leukemias (AML) has been recently unraveled. However, due to their genetic heterogeneity, only a handful of markers are currently used for the evaluation of minimal residual disease (MRD). Recent studies using multi-target strategies indicate that detection of residual mutations in less than 5% of cells in complete remission is associated with a better survival. Here, in a series of 69 AMLs with known clonal architecture, we design a clone-specific strategy based on fluorescent hybridization and high-sensitivity next generation sequencing to detect chromosomal aberrations and mutations, respectively, in follow-up samples. The combination of these techniques allows tracking chromosomal and genomic lesions down to 0.5-0.4% of the cell population in remission samples. By testing all lesions in follow-up samples from 65 of 69 evaluable patients, we find that initiating events often persist and appear to be, on their own, inappropriate markers to predict short-term relapse. In contrast, the persistence of two or more lesions in more than 0.4% of the cells from remission samples is strongly associated with lower leukemia-free and overall survivals in univariate and multivariate analyses. Although larger prospective studies are needed to extend these results, our data show that a personalized, clone-specific, MRD follow up strategy is feasible in the vast majority of AML cases.

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