Leukemic Blasts in Transformed JAK2-V617F-positive Myeloproliferative Disorders Are Frequently Negative for the JAK2-V617F Mutation

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2007 Mar 17

PMID 17363731

Citations 105

Authors

Alexandre Theocharides

Marjorie Boissinot

Francois Girodon

Richard Garand

Soon-Siong Teo

Eric Lippert

Pascaline Talmant

Andre Tichelli

Sylvie Hermouet

Radek C Skoda

Affiliations

Soon will be listed here.

Abstract

To study the role of the JAK2-V617F mutation in leukemic transformation, we examined 27 patients with myeloproliferative disorders (MPDs) who transformed to acute myeloid leukemia (AML). At MPD diagnosis, JAK2-V617F was detectable in 17 of 27 patients. Surprisingly, only 5 of 17 patients developed JAK2-V617F-positive AML, whereas 9 of 17 patients transformed to JAK2-V617F-negative AML. Microsatellite analysis in a female patient showed that mitotic recombination was not responsible for the transition from JAK2-V617F-positive MPD to JAK2-V617F-negative AML, and clonality determined by the MPP1 polymorphism demonstrated that the granulocytes and leukemic blasts inactivated the same parental X chromosome. In a second patient positive for JAK2-V617F at transformation, but with JAK2-V617F-negative leukemic blasts, we found del(11q) in all cells examined, suggesting a common clonal origin of MPD and AML. We conclude that JAK2-V617F-positive MPD frequently yields JAK2-V617F-negative AML, and transformation of a common JAK2-V617F-negative ancestor represents a possible mechanism.

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