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TEL-AML1 通过 microRNA-494 和 microRNA-320a 调控存活素和细胞凋亡。

TEL-AML1 regulation of survivin and apoptosis via miRNA-494 and miRNA-320a.

机构信息

Laboratory for Molecular Epidemiology, University of California, San Francisco, San Francisco, CA, USA.

出版信息

Blood. 2010 Dec 2;116(23):4885-93. doi: 10.1182/blood-2009-02-206706. Epub 2010 Aug 31.

Abstract

There is increasing evidence that miRNA and transcription factors interact in an instructive fashion in normal and malignant hematopoiesis. We explored the impact of TEL-AML1 (ETV6-RUNX1), the most common fusion protein in childhood leukemia, on miRNA expression and the leukemic phenotype. Using RNA interference, miRNA expression arrays, and quantitative polymerase chain reaction, we identified miRNA-494 and miRNA-320a to be up-regulated upon TEL-AML1 silencing independently of TEL expression. Chromatin immunoprecipitation analysis identified miRNA-494 as a direct miRNA target of the fusion protein TEL-AML1. Using bioinformatic analysis as well as functional luciferase experiments, we demonstrate that survivin is a target of the 2 miRNAs. miRNA-494 and miRNA-320a were introduced to the cells by transfection and survivin expression determined by Western blot analysis. These miRNAs blocked survivin expression and resulted in apoptosis in a similar manner as TEL-AML1 silencing by itself; this silencing was also shown to be Dicer-dependent. miRNAs-494 and -320a are expressed at lower levels in TEL-AML1+ leukemias compared with immunophenotype-matched nonTEL-AML1 acute lymphoblastic leukemia subtypes, and within TEL-AML1+ leukemias their expression is correlated to survivin levels. In summary our data suggest that TEL-AML1 might exert its antiapoptotic action at least in part by suppressing miRNA-494 and miRNA-320a, lowering their expression causing enhanced survivin expression.

摘要

越来越多的证据表明,miRNA 和转录因子在正常和恶性造血中以一种有指导意义的方式相互作用。我们探讨了 TEL-AML1(ETV6-RUNX1),即儿童白血病中最常见的融合蛋白,对 miRNA 表达和白血病表型的影响。通过 RNA 干扰、miRNA 表达谱和定量聚合酶链反应,我们发现 TEL-AML1 沉默后,miRNA-494 和 miRNA-320a 独立于 TEL 表达而上调。染色质免疫沉淀分析确定 miRNA-494 是融合蛋白 TEL-AML1 的直接 miRNA 靶标。通过生物信息学分析和功能荧光素酶实验,我们证明 survivin 是这 2 个 miRNA 的靶标。通过转染将 miRNA-494 和 miRNA-320a 引入细胞,并通过 Western blot 分析确定 survivin 表达。这些 miRNA 阻断 survivin 表达,并以类似于 TEL-AML1 沉默本身的方式导致细胞凋亡;这种沉默也依赖于 Dicer。与免疫表型匹配的非 TEL-AML1 急性淋巴细胞白血病亚型相比,TEL-AML1+白血病中 miRNA-494 和 miRNA-320a 的表达水平较低,而在 TEL-AML1+白血病中,其表达与 survivin 水平相关。总之,我们的数据表明,TEL-AML1 可能通过抑制 miRNA-494 和 miRNA-320a 来发挥其抗凋亡作用,降低其表达水平导致 survivin 表达增强。

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