Single-cell Sequencing Reveals the Origin and the Order of Mutation Acquisition in T-cell Acute Lymphoblastic Leukemia

Overview

Journal Leukemia

Specialties Hematology
Oncology

Date 2018 May 10

PMID 29740158

Citations 48

Authors

Jolien De Bie

Sofie Demeyer

Llucia Alberti-Servera

Ellen Geerdens

Heidi Segers

Michael Broux

Kim De Keersmaecker

Lucienne Michaux

Peter Vandenberghe

Thierry Voet

Nancy Boeckx

Anne Uyttebroeck

Jan Cools

Affiliations

Soon will be listed here.

Abstract

Next-generation sequencing has provided a detailed overview of the various genomic lesions implicated in the pathogenesis of T-cell acute lymphoblastic leukemia (T-ALL). Typically, 10-20 protein-altering lesions are found in T-ALL cells at diagnosis. However, it is currently unclear in which order these mutations are acquired and in which progenitor cells this is initiated. To address these questions, we used targeted single-cell sequencing of total bone marrow cells and CD34CD38 multipotent progenitor cells for four T-ALL cases. Hierarchical clustering detected a dominant leukemia cluster at diagnosis, accompanied by a few smaller clusters harboring only a fraction of the mutations. We developed a graph-based algorithm to determine the order of mutation acquisition. Two of the four patients had an early event in a known oncogene (MED12, STAT5B) among various pre-leukemic events. Intermediate events included loss of 9p21 (CDKN2A/B) and acquisition of fusion genes, while NOTCH1 mutations were typically late events. Analysis of CD34CD38 cells and myeloid progenitors revealed that in half of the cases somatic mutations were detectable in multipotent progenitor cells. We demonstrate that targeted single-cell sequencing can elucidate the order of mutation acquisition in T-ALL and that T-ALL development can start in a multipotent progenitor cell.

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