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一种含有 AF4 和 ENL 家族蛋白与 P-TEFb 的更高阶复合物,促进了致癌和生理上依赖 MLL 的转录。

A higher-order complex containing AF4 and ENL family proteins with P-TEFb facilitates oncogenic and physiologic MLL-dependent transcription.

机构信息

National Cancer Center Research Institute, Tokyo, Japan.

出版信息

Cancer Cell. 2010 Feb 17;17(2):198-212. doi: 10.1016/j.ccr.2009.12.040.

DOI:10.1016/j.ccr.2009.12.040
PMID:20153263
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2824033/
Abstract

AF4 and ENL family proteins are frequently fused with MLL, and they comprise a higher order complex (designated AEP) containing the P-TEFb transcription elongation factor. Here, we show that AEP is normally recruited to MLL-target chromatin to facilitate transcription. In contrast, MLL oncoproteins fused with AEP components constitutively form MLL/AEP hybrid complexes to cause sustained target gene expression, which leads to transformation of hematopoietic progenitors. Furthermore, MLL-AF6, an MLL fusion with a cytoplasmic protein, does not form such hybrid complexes, but nevertheless constitutively recruits AEP to target chromatin via unknown alternative mechanisms. Thus, AEP recruitment is an integral part of both physiological and pathological MLL-dependent transcriptional pathways. Bypass of its normal recruitment mechanisms is the strategy most frequently used by MLL oncoproteins.

摘要

AF4 和 ENL 家族蛋白常与 MLL 融合,它们构成一个包含 P-TEFb 转录延伸因子的高级复合物(命名为 AEP)。在这里,我们表明 AEP 通常被募集到 MLL 靶染色质以促进转录。相比之下,与 AEP 成分融合的 MLL 癌蛋白组成性地形成 MLL/AEP 杂合复合物,导致持续的靶基因表达,从而导致造血祖细胞的转化。此外,与细胞质蛋白融合的 MLL-AF6 不形成这种杂合复合物,但仍通过未知的替代机制组成性地将 AEP 募集到靶染色质。因此,AEP 的募集是 MLL 依赖性转录途径的生理和病理过程的一个组成部分。MLL 癌蛋白最常使用的策略是绕过其正常募集机制。

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