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MRG结构域多特异性的结构基础。

Structural Basis for Multi-specificity of MRG Domains.

作者信息

Xie Tao, Zmyslowski Adam M, Zhang Yongbo, Radhakrishnan Ishwar

机构信息

Department of Molecular Biosciences, Northwestern University, Evanston, IL 60208, USA.

Department of Chemistry, Northwestern University, Evanston, IL 60208, USA.

出版信息

Structure. 2015 Jun 2;23(6):1049-57. doi: 10.1016/j.str.2015.03.020. Epub 2015 May 7.

Abstract

Chromatin-binding proteins play vital roles in the assembly and recruitment of multi-subunit complexes harboring effector proteins to specific genomic loci. MRG15, a chromodomain-containing chromatin-binding protein, recruits diverse chromatin-associated complexes that regulate gene transcription, DNA repair, and RNA splicing. Previous studies with Pf1, another chromatin-binding subunit of the Sin3S/Rpd3S histone deacetylase complex, defined the sequence and structural requirements for interactions with the MRG15 MRG domain, a common target of diverse subunits in the aforementioned complexes. We now show that MRGBP, a member of the Tip60/NuA4 histone acetyltransferase complex, engages the same two surfaces of the MRG domain as Pf1. High-affinity interactions occur via a bipartite structural motif including an FxLP sequence motif. MRGBP shares little sequence and structural similarity with Pf1, yet targets similar pockets on the surface of the MRG domain, mimicking Pf1 in its interactions. Our studies shed light onto how MRG domains have evolved to bind diverse targets.

摘要

染色质结合蛋白在将含有效应蛋白的多亚基复合物组装并募集到特定基因组位点的过程中发挥着至关重要的作用。MRG15是一种含染色质结构域的染色质结合蛋白,它募集多种与染色质相关的复合物,这些复合物可调节基因转录、DNA修复和RNA剪接。先前对Sin3S/Rpd3S组蛋白去乙酰化酶复合物的另一个染色质结合亚基Pf1的研究,确定了与MRG15的MRG结构域相互作用的序列和结构要求,MRG15的MRG结构域是上述复合物中多种亚基的共同靶点。我们现在表明,Tip60/NuA4组蛋白乙酰转移酶复合物的成员MRGBP与Pf1结合MRG结构域的相同两个表面。高亲和力相互作用通过一个包括FxLP序列基序的二分结构基序发生。MRGBP与Pf1在序列和结构上几乎没有相似性,但靶向MRG结构域表面的相似口袋,在相互作用中模仿Pf1。我们的研究揭示了MRG结构域是如何进化以结合不同靶点的。

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