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C 末端结合蛋白核心抑制因子的保守催化和 C 末端调节结构域精细调节了发育过程中的转录反应。

Conserved catalytic and C-terminal regulatory domains of the C-terminal binding protein corepressor fine-tune the transcriptional response in development.

机构信息

Department of Biochemistry and Molecular Biology, Michigan State University, 413 Biochemistry, East Lansing, MI 48824-1319, USA.

出版信息

Mol Cell Biol. 2011 Jan;31(2):375-84. doi: 10.1128/MCB.00772-10. Epub 2010 Nov 15.

Abstract

Transcriptional corepressors play complex roles in developmental gene regulation. These proteins control transcription by recruiting diverse chromatin-modifying enzymes, but it is not known whether corepressor activities are finely regulated in different developmental settings or whether their basic activities are identical in most contexts. The evolutionarily conserved C-terminal binding protein (CtBP) is recruited by a variety of transcription factors that play crucial roles in development and disease. CtBP contains a central NAD(H) binding core domain that is homologous to D2 hydroxy acid dehydrogenase enzymes, as well as an unstructured C-terminal domain. NAD(H) binding is important for CtBP function, but the significance of its intrinsic dehydrogenase activity, as well as that of the unstructured C terminus, is poorly understood. To clarify the biological relevance of these features, we established genetic rescue assays to determine how different forms of CtBP function in the context of Drosophila melanogaster development. The mutant phenotypes and specific gene regulatory effects indicate that both the catalytic site of CtBP and the C-terminal extension play important, if nonessential roles in development. Our results indicate that the structural and enzymatic features of CtBP, previously thought to be dispensable for overall transcriptional control, are critical for modulating this protein's activity in diverse developmental settings.

摘要

转录共抑制因子在发育基因调控中发挥着复杂的作用。这些蛋白通过招募多种染色质修饰酶来控制转录,但目前尚不清楚共抑制因子的活性是否在不同的发育环境中得到精细调节,或者它们在大多数情况下的基本活性是否相同。进化上保守的 C 端结合蛋白(CtBP)被多种在发育和疾病中发挥关键作用的转录因子募集。CtBP 包含一个中央 NAD(H)结合核心结构域,与 D2 羟酸脱氢酶酶同源,以及一个无结构的 C 端结构域。NAD(H)结合对 CtBP 功能很重要,但它的内在脱氢酶活性以及无结构 C 端的意义尚不清楚。为了阐明这些特征的生物学相关性,我们建立了遗传挽救测定来确定不同形式的 CtBP 在黑腹果蝇发育中的功能。突变表型和特定的基因调控效应表明,CtBP 的催化位点和 C 端延伸都在发育中发挥重要作用(尽管不是必需的)。我们的结果表明,先前认为对整体转录控制可有可无的 CtBP 的结构和酶学特征对于调节该蛋白在不同发育环境中的活性至关重要。

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