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SANT结构域在多种染色质重塑酶功能发挥中起关键作用。

Essential role for the SANT domain in the functioning of multiple chromatin remodeling enzymes.

作者信息

Boyer Laurie A, Langer Michael R, Crowley Kimberly A, Tan Song, Denu John M, Peterson Craig L

机构信息

Program in Molecular Medicine, University of Massachusetts Medical School, Worcester, MA 01605, USA.

出版信息

Mol Cell. 2002 Oct;10(4):935-42. doi: 10.1016/s1097-2765(02)00634-2.

Abstract

The SANT domain is a novel motif found in a number of eukaryotic transcriptional regulatory proteins that was identified based on its homology to the DNA binding domain of c-myb. Here we show that the SANT domain is essential for the in vivo functions of yeast Swi3p, Ada2p, and Rsc8p, subunits of three distinct chromatin remodeling complexes. We also find that the Ada2p SANT domain is essential for histone acetyltransferase activity of native, Gcn5p-containing HAT complexes. Furthermore, kinetic analyses indicate that an intact SANT domain is required for an Ada2p-dependent enhancement of histone tail binding and enzymatic catalysis by Gcn5p. Our results are consistent with a general role for SANT domains in functional interactions with histone N-terminal tails.

摘要

SANT结构域是在许多真核转录调节蛋白中发现的一种新基序,它是基于与c-myb的DNA结合结构域的同源性而被鉴定出来的。在这里,我们表明SANT结构域对于酵母Swi3p、Ada2p和Rsc8p这三种不同染色质重塑复合物亚基的体内功能至关重要。我们还发现,Ada2p的SANT结构域对于天然含Gcn5p的组蛋白乙酰转移酶复合物的组蛋白乙酰转移酶活性至关重要。此外,动力学分析表明,完整的SANT结构域是Gcn5p依赖的组蛋白尾部结合增强和酶催化所必需的。我们的结果与SANT结构域在与组蛋白N端尾部功能相互作用中的一般作用一致。

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