Department of Biological Sciences, Korea Advanced Institute of Science and Technology (KAIST), KAIST Institute of BioCentury, Daejeon 34141, Korea.
Department of Physics and Astronomy, Institute of Applied Physics, Seoul National University, Seoul 08826, Korea.
J Mol Biol. 2021 Sep 3;433(18):167114. doi: 10.1016/j.jmb.2021.167114. Epub 2021 Jun 21.
Chromodomain-Helicase DNA binding protein 7 (CHD7) is an ATP dependent chromatin remodeler involved in maintaining open chromatin structure. Mutations of CHD7 gene causes multiple developmental disorders, notably CHARGE syndrome. However, there is not much known about the molecular mechanism by which CHD7 remodels nucleosomes. Here, we performed biochemical and biophysical analysis on CHD7 chromatin remodeler and uncover that N-terminal to the Chromodomain (N-CRD) interacts with nucleosome and contains a high conserved arginine stretch, which is reminiscent of arginine anchor. Importantly, this region is required for efficient ATPase stimulation and nucleosome remodeling activity of CHD7. Furthermore, smFRET analysis shows the mutations in the N-CRD causes the defects in remodeling activity. Collectively, our results uncover the functional importance of a previously unidentified N-terminal region in CHD7 and implicate that the multiple domains in chromatin remodelers are involved in regulating their activities.
染色质解旋酶 DNA 结合蛋白 7(CHD7)是一种依赖于 ATP 的染色质重塑酶,参与维持开放染色质结构。CHD7 基因突变会导致多种发育障碍,特别是 CHARGE 综合征。然而,关于 CHD7 重塑核小体的分子机制还知之甚少。在这里,我们对 CHD7 染色质重塑酶进行了生化和生物物理分析,揭示了染色质域(N-CRD)的 N 端与核小体相互作用,并含有一个高度保守的精氨酸延伸,使人联想到精氨酸锚。重要的是,该区域对于 CHD7 的高效 ATP 酶刺激和核小体重塑活性是必需的。此外,smFRET 分析表明,N-CRD 中的突变会导致重塑活性缺陷。总之,我们的研究结果揭示了 CHD7 中一个以前未被识别的 N 端区域的功能重要性,并表明染色质重塑酶的多个结构域参与调节它们的活性。
Zotero 插件