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连接组蛋白H5及其球状结构域的自我缔合:特定自我接触的证据。

Self-association of linker histone H5 and of its globular domain: evidence for specific self-contacts.

作者信息

Carter G J, van Holde K

机构信息

Department of Biochemistry and Biophysics, Oregon State University, Corvallis 97331-7305, USA.

出版信息

Biochemistry. 1998 Sep 8;37(36):12477-88. doi: 10.1021/bi980716v.

Abstract

The ability of avian-specific linker histone H5, and the globular domains of H5 (GH5) and H1(0) (GH1(0), to self-associate either free in solution or when bound to DNA was investigated. All three proteins underwent a salt-dependent increase in turbidity that may be indicative of nonspecific interactions. Dithiobis(succinimidyl propionate) cross-linking was used to measure specific contacts for both H5 and GH5 free in solution and bound to DNA. H5 and GH5 each became cross-linked in solution, with GH5 displaying divalent polymerization interactions, which suggests that two specific surfaces were involved in the assembly process. For GH5-DNA complexes, cross-linking appeared to be largely the consequence of aggregation, but under low concentrations of DSP, cross-linking GH5 was observed to assemble preferentially onto DNA before oligomerizing to form massive aggregates. Both linear and supercoiled DNA facilitated GH5 interactions compared to assembly in solution; differences in the distribution of cross-linked polymer sizes indicates that assembly is dependent on both the presence of DNA and the morphology of the DNA. Finally, on the basis of a technique referred to as quantitative proteolysis, GH5 assembly on DNA appears to involve specific protein-protein contacts involving the C terminus of one partner. Overall, the cumulative results reported here support the premise that linker histones assemble specifically both in solution and on DNA.

摘要

研究了禽类特异性连接组蛋白H5、H5的球状结构域(GH5)和H1(0)的球状结构域(GH1(0))在溶液中游离或与DNA结合时的自缔合能力。所有这三种蛋白质的浊度都随盐浓度增加,这可能表明存在非特异性相互作用。使用二硫代双(琥珀酰亚胺丙酸酯)交联来测量溶液中游离的以及与DNA结合的H5和GH5的特异性接触。H5和GH5在溶液中均发生交联,GH5表现出二价聚合相互作用,这表明在组装过程中有两个特定表面参与。对于GH5-DNA复合物,交联似乎主要是聚集的结果,但在低浓度的DSP下,观察到交联的GH5在寡聚形成大量聚集体之前优先组装到DNA上。与在溶液中组装相比,线性和超螺旋DNA都促进了GH5的相互作用;交联聚合物大小分布的差异表明组装既取决于DNA的存在,也取决于DNA的形态。最后,基于一种称为定量蛋白水解的技术,GH5在DNA上的组装似乎涉及特定的蛋白质-蛋白质接触,其中一个伴侣的C末端参与其中。总体而言,此处报告的累积结果支持连接组蛋白在溶液中和在DNA上均特异性组装的前提。

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