Genomic and functional analysis of leukemic transformation of myeloproliferative neoplasms

鲁索利替尼 癌症研究 髓样 髓系白血病 医学 祖细胞 癸他滨 人口 肿瘤科 内科学 免疫学 生物 骨髓 干细胞 骨髓纤维化 遗传学 基因 基因表达 环境卫生 DNA甲基化
作者
Raajit K. Rampal,Jihae Ahn,Omar Abdel-Wahab,Michelle Nahas,Kai Wang,Doron Lipson,Geoff Otto,Roman Yelensky,Todd Hricik,Anna Sophia McKenney,Gabriela Chiosis,Young Rock Chung,Suveg Pandey,Marcel R.M. van den Brink,Scott A. Armstrong,Ahmet Doğan,Andrew M. Intlekofer,Taghi Manshouri,Christopher Y. Park,Srđan Verstovšek,Franck Rapaport,Philip J. Stephens,Vincent A. Miller,Ross L. Levine
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [National Academy of Sciences]
卷期号:111 (50) 被引量:234
标识
DOI:10.1073/pnas.1407792111
摘要

Patients with myeloproliferative neoplasms (MPNs) are at significant, cumulative risk of leukemic transformation to acute myeloid leukemia (AML), which is associated with adverse clinical outcome and resistance to standard AML therapies. We performed genomic profiling of post-MPN AML samples; these studies demonstrate somatic tumor protein 53 (TP53) mutations are common in JAK2V617F-mutant, post-MPN AML but not in chronic-phase MPN and lead to clonal dominance of JAK2V617F/TP53-mutant leukemic cells. Consistent with these data, expression of JAK2V617F combined with Tp53 loss led to fully penetrant AML in vivo. JAK2V617F-mutant, Tp53-deficient AML was characterized by an expanded megakaryocyte erythroid progenitor population that was able to propagate the disease in secondary recipients. In vitro studies revealed that post-MPN AML cells were sensitive to decitabine, the JAK1/2 inhibitor ruxolitinib, or the heat shock protein 90 inhibitor 8-(6-iodobenzo[d][1.3]dioxol-5-ylthio)-9-(3-(isopropylamino)propyl)-9H-purine-6-amine (PU-H71). Treatment with ruxolitinib or PU-H71 improved survival of mice engrafted with JAK2V617F-mutant, Tp53-deficient AML, demonstrating therapeutic efficacy for these targeted therapies and providing a rationale for testing these therapies in post-MPN AML.

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