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在核小体阵列的折叠和寡聚化过程中,H4尾部结构域参与了与蛋白质和DNA的核小体内及核小体间相互作用。

The H4 tail domain participates in intra- and internucleosome interactions with protein and DNA during folding and oligomerization of nucleosome arrays.

作者信息

Kan Pu-Yeh, Caterino Tamara L, Hayes Jeffrey J

机构信息

Department of Pathology, University of Rochester, Rochester, New York 14642, USA.

出版信息

Mol Cell Biol. 2009 Jan;29(2):538-46. doi: 10.1128/MCB.01343-08. Epub 2008 Nov 10.

Abstract

The condensation of nucleosome arrays into higher-order secondary and tertiary chromatin structures likely involves long-range internucleosomal interactions mediated by the core histone tail domains. We have characterized interarray interactions mediated by the H4 tail domain, known to play a predominant role in the formation of such structures. We find that the N-terminal end of the H4 tail mediates interarray contacts with DNA during self-association of oligonucleosome arrays similar to that found previously for the H3 tail domain. However, a site near the histone fold domain of H4 participates in a distinct set of interactions, contacting both DNA and H2A in condensed structures. Moreover, we also find that H4-H2A interactions occur via an intra- as well as an internucleosomal fashion, supporting an additional intranucleosomal function for the tail. Interestingly, acetylation of the H4 tail has little effect on interarray interactions by itself but overrides the strong stimulation of interarray interactions induced by linker histones. Our results indicate that the H4 tail facilitates secondary and tertiary chromatin structure formation via a complex array of potentially exclusive interactions that are distinct from those of the H3 tail domain.

摘要

核小体阵列凝聚成更高阶的二级和三级染色质结构可能涉及由核心组蛋白尾部结构域介导的长程核小体间相互作用。我们已经对由H4尾部结构域介导的阵列间相互作用进行了表征,已知该结构域在这类结构的形成中起主要作用。我们发现,在寡核小体阵列的自组装过程中,H4尾部的N末端介导了与DNA的阵列间接触,这与之前在H3尾部结构域中发现的情况类似。然而,H4组蛋白折叠结构域附近的一个位点参与了一组不同的相互作用,在凝聚结构中与DNA和H2A都有接触。此外,我们还发现H4与H2A的相互作用以核小体内和核小体间的方式发生,这支持了尾部的额外核小体内功能。有趣的是,H4尾部的乙酰化本身对阵列间相互作用影响很小,但会抵消连接组蛋白对阵列间相互作用的强烈刺激。我们的结果表明,H4尾部通过一系列复杂的、可能相互排斥的相互作用促进二级和三级染色质结构的形成,这些相互作用与H3尾部结构域的相互作用不同。

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