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由c-MYC致癌网络激活的SIRT1促进人FLT3-ITD急性髓系白血病干细胞的维持和耐药性。

SIRT1 activation by a c-MYC oncogenic network promotes the maintenance and drug resistance of human FLT3-ITD acute myeloid leukemia stem cells.

作者信息

Li Ling, Osdal Tereza, Ho Yinwei, Chun Sookhee, McDonald Tinisha, Agarwal Puneet, Lin Allen, Chu Su, Qi Jing, Li Liang, Hsieh Yao-Te, Dos Santos Cedric, Yuan Hongfeng, Ha Trung-Quang, Popa Mihaela, Hovland Randi, Bruserud Øystein, Gjertsen Bjørn Tore, Kuo Ya-Huei, Chen Wenyong, Lain Sonia, McCormack Emmet, Bhatia Ravi

机构信息

Division of Hematopoietic Stem Cell and Leukemia Research, City of Hope National Medical Center, Duarte, CA 91010, USA.

Department of Clinical Science, Hematology Section, University of Bergen, Bergen 5021, Norway.

出版信息

Cell Stem Cell. 2014 Oct 2;15(4):431-446. doi: 10.1016/j.stem.2014.08.001.

DOI:10.1016/j.stem.2014.08.001
PMID:25280219
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4305398/
Abstract

The FLT3-ITD mutation is frequently observed in acute myeloid leukemia (AML) and is associated with poor prognosis. In such patients, FLT3 tyrosine kinase inhibitors (TKIs) are only partially effective and do not eliminate the leukemia stem cells (LSCs) that are assumed to be the source of treatment failure. Here, we show that the NAD-dependent SIRT1 deacetylase is selectively overexpressed in primary human FLT3-ITD AML LSCs. This SIRT1 overexpression is related to enhanced expression of the USP22 deubiquitinase induced by c-MYC, leading to reduced SIRT1 ubiquitination and enhanced stability. Inhibition of SIRT1 expression or activity reduced the growth of FLT3-ITD AML LSCs and significantly enhanced TKI-mediated killing of the cells. Therefore, these results identify a c-MYC-related network that enhances SIRT1 protein expression in human FLT3-ITD AML LSCs and contributes to their maintenance. Inhibition of this oncogenic network could be an attractive approach for targeting FLT3-ITD AML LSCs to improve treatment outcomes.

摘要

FLT3-ITD突变在急性髓系白血病(AML)中经常被观察到,并且与预后不良相关。在这类患者中,FLT3酪氨酸激酶抑制剂(TKIs)仅部分有效,并且不能消除被认为是治疗失败根源的白血病干细胞(LSCs)。在此,我们表明NAD依赖的SIRT1去乙酰化酶在原发性人类FLT3-ITD AML LSCs中选择性过表达。这种SIRT1过表达与c-MYC诱导的USP22去泛素酶表达增强有关,导致SIRT1泛素化减少和稳定性增强。抑制SIRT1表达或活性可降低FLT3-ITD AML LSCs的生长,并显著增强TKI介导的细胞杀伤作用。因此,这些结果确定了一个与c-MYC相关的网络,该网络增强了人类FLT3-ITD AML LSCs中SIRT1蛋白表达并有助于其维持。抑制这个致癌网络可能是靶向FLT3-ITD AML LSCs以改善治疗结果的一种有吸引力的方法。

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