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Activating mutations in human acute megakaryoblastic leukemia
Authors:Malinge Sébastien  Ragu Christine  Della-Valle Veronique  Pisani Didier  Constantinescu Stefan N  Perez Christelle  Villeval Jean-Luc  Reinhardt Dirk  Landman-Parker Judith  Michaux Lucienne  Dastugue Nicole  Baruchel André  Vainchenker William  Bourquin Jean-Pierre  Penard-Lacronique Virginie  Bernard Olivier A
Affiliation:Institut National de la Santé et de la Recherche Scientifique (INSERM), E0210, Paris, France.
Abstract:Oncogenic activation of tyrosine kinase signaling pathway is recurrent in human leukemia. To gain insight into the oncogenic process leading to acute megakaryoblastic leukemia (AMKL), we performed sequence analyses of a subset of oncogenes known to be activated in human myeloid and myeloproliferative disorders. In a series of human AMKL samples from both Down syndrome and non-Down syndrome patients, mutations were identified within KIT, FLT3, JAK2, JAK3, and MPL genes, with a higher frequency in DS than in non-DS patients. The novel mutations were analyzed using BaF3 cells, showing that JAK3 mutations were activating mutations. Finally, we report a novel constitutively active MPL mutant, MPLT487A, observed in a non-Down syndrome childhood AMKL that induces a myeloproliferative disease in mouse bone marrow transplantation assay.
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