Myc诱导的B细胞淋巴瘤中微小RNA的miR-17~92簇的遗传学剖析

Genetic dissection of the miR-17~92 cluster of microRNAs in Myc-induced B-cell lymphomas.

作者信息

Mu Ping, Han Yoon-Chi, Betel Doron, Yao Evelyn, Squatrito Massimo, Ogrodowski Paul, de Stanchina Elisa, D'Andrea Aleco, Sander Chris, Ventura Andrea

机构信息

Cancer Biology and Genetics Program, Memorial Sloan Kettering Cancer Center, New York, New York 10021, USA.

出版信息

Genes Dev. 2009 Dec 15;23(24):2806-11. doi: 10.1101/gad.1872909.

DOI:10.1101/gad.1872909

PMID:20008931

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2800095/

Abstract

The miR-17 approximately 92 cluster is frequently amplified or overexpressed in human cancers and has emerged as the prototypical oncogenic polycistron microRNA (miRNA). miR-17 approximately 92 is a direct transcriptional target of c-Myc, and experiments in a mouse model of B-cell lymphomas have shown cooperation between these two oncogenes. However, both the molecular mechanism underlying this cooperation and the individual miRNAs that are responsible for it are unknown. By using a conditional knockout allele of miR-17 approximately 92, we show here that sustained expression of endogenous miR-17 approximately 92 is required to suppress apoptosis in Myc-driven B-cell lymphomas. Furthermore, we show that among the six miRNAs that are encoded by miR-17 approximately 92, miR-19a and miR-19b are absolutely required and largely sufficient to recapitulate the oncogenic properties of the entire cluster. Finally, by combining computational target prediction, gene expression profiling, and an in vitro screening strategy, we identify a subset of miR-19 targets that mediate its prosurvival activity.

摘要

miR-17~~92簇在人类癌症中经常发生扩增或过表达，并已成为典型的致癌多顺反子微小RNA（miRNA）。miR-17~~92是c-Myc的直接转录靶点，在B细胞淋巴瘤小鼠模型中的实验表明这两个致癌基因之间存在协同作用。然而，这种协同作用的分子机制以及负责此作用的单个miRNA均尚不清楚。通过使用miR-17~~92的条件性敲除等位基因，我们在此表明，在Myc驱动的B细胞淋巴瘤中，内源性miR-17~~92的持续表达是抑制细胞凋亡所必需的。此外，我们表明，在由miR-17~92编码的6个miRNA中，miR-19a和miR-19b是绝对必需的，并且在很大程度上足以重现整个簇的致癌特性。最后，通过结合计算靶点预测、基因表达谱分析和体外筛选策略，我们鉴定出介导其促生存活性的miR-19靶点子集。

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