Corepressors: custom tailoring and alterations while you wait.

Nuclear receptor signaling Pub Date : 2005-01-01 Epub Date: 2005-10-21 DOI:10.1621/nrs.03003

Michael Goodson, Brian A Jonas, Martin A Privalsky

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引用次数: 72

Abstract

A diverse cadre of metazoan transcription factors mediate repression by recruiting protein complexes containing the SMRT (silencing mediator of retinoid and thyroid hormone receptor) or N-CoR (nuclear receptor corepressor) corepressors. SMRT and N-CoR nucleate the assembly of still larger corepressor complexes that perform the specific molecular incantations necessary to confer transcriptional repression. Although SMRT and N-CoR are paralogs and possess similar molecular architectures and mechanistic strategies, they nonetheless exhibit distinct molecular and biological properties. It is now clear that the functions of both SMRT and N-CoR are further diversified through alternative mRNA splicing, yielding a series of corepressor protein variants that participate in distinctive transcription factor partnerships and display distinguishable repression properties. This review will discuss what is known about the structure and actions of SMRT, N-CoR, and their splicing variants, and how alternative splicing may allow the functions of these corepressors to be adapted and tailored to different cells and to different developmental stages.

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协阻遏器:定制剪裁和改变，而你等待。

多种后生动物转录因子通过招募含有SMRT(类视黄醇和甲状腺激素受体沉默介质)或N-CoR(核受体辅抑制因子)辅抑制因子的蛋白复合物来介导抑制。SMRT和N-CoR构成更大的辅抑制子复合物的装配核，这些复合物执行赋予转录抑制所必需的特定分子咒语。虽然SMRT和N-CoR是同源的，具有相似的分子结构和机制策略，但它们仍然表现出不同的分子和生物学特性。现在清楚的是，SMRT和N-CoR的功能通过可选的mRNA剪接进一步多样化，产生一系列参与不同转录因子伙伴关系并显示不同抑制特性的辅抑制蛋白变体。本文将讨论SMRT、N-CoR及其剪接变体的结构和作用，以及选择性剪接如何使这些共阻遏子的功能适应不同的细胞和不同的发育阶段。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Nuclear receptor signaling

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