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Implications of the miR-10 family in chemotherapy response of NPM1-mutated AML

机译:MIR-10家族在NPM1 - 突变AML化疗反应中的影响

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摘要

Nucleophosmin-mutated acute myeloid leukemia (NPM1mut-AML) patients have a high rate of complete remission (CR) to induction chemotherapy. However, the mechanisms responsible for such effects are unknown. BecausemiR-10 family members are expressed at high levels in NPM1mut-AML, we evaluated whether these microRNAs could predict chemotherapy response in AML. We found that high baseline miR-10 family expression in 54 untreated cytogenetically heterogeneous AML patients was associated with achieving CR. However, when we included NPM1 mutation status in the multivariable model, there was a significant interaction effect between miR-10a-5p expression and NPM1 mutation status. Similar results were observed when using a second cohort of 183 cytogenetically normal older (age >= 60 years) AML patients. Loss-and gain-of-function experiments using miR-10a-5p in cell lines and primary blasts did not demonstrate any effect in apoptosis or cell proliferation at baseline or after chemotherapy. These data support a bystander role for the miR-10 family in NPM1mut-AML.
机译:Nucleophosmin-突变的急性髓性白血病(NPM1MUT-AML)患者具有高完全缓解(CR)的高速率化疗。然而,对这种效果负责的机制是未知的。 BECAUSEMIR-10家族成员在NPM1MUT-AML的高水平表达,我们评估了这些MICRRNAS是否可以预测AML中的化疗反应。我们发现,54个未处理的细胞异质非均质AML患者的高基线miR-10系列表达与实现Cr相关。然而,当我们在多变量模型中包括NPM1突变状态时,MIR-10A-5P表达和NPM1突变状态之间存在显着的相互作用效果。使用第二次群组183个细胞常规较大的较大(年龄> = 60岁)AML患者时观察到类似的结果。使用MiR-10a-5p在细胞系和原发性爆炸中使用MiR-10a-5p的丧失和函数的实验未表明基线或化疗后的凋亡或细胞增殖中的任何效果。这些数据支持在NPM1MUT-AML中MIR-10系列的旁观者角色。

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