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肌动蛋白加帽蛋白生化功能的 CPI 基序调控的比较分析

Comparative Analysis of CPI-Motif Regulation of Biochemical Functions of Actin Capping Protein.

机构信息

Department of Biochemistry and Molecular Biophysics, Washington University School of Medicine, St. Louis, Missouri 63110, United States.

出版信息

Biochemistry. 2020 Mar 24;59(11):1202-1215. doi: 10.1021/acs.biochem.0c00092. Epub 2020 Mar 10.

DOI:10.1021/acs.biochem.0c00092
PMID:32133840
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7301643/
Abstract

The heterodimeric actin capping protein (CP) is regulated by a set of proteins that contain CP-interacting (CPI) motifs. Outside of the CPI motif, the sequences of these proteins are unrelated and distinct. The CPI motif and surrounding sequences are conserved within a given protein family, when compared to those of other CPI-motif protein families. Using biochemical assays with purified proteins, we compared the ability of CPI-motif-containing peptides from different protein families (a) to bind to CP, (b) to allosterically inhibit barbed-end capping by CP, and (c) to allosterically inhibit interaction of CP with V-1, another regulator of CP. We found large differences in potency among the different CPI-motif-containing peptides, and the different functional assays showed different orders of potency. These biochemical differences among the CPI-motif peptides presumably reflect interactions between CP and CPI-motif peptides involving amino acid residues that are conserved but are not part of the strictly defined consensus, as it was originally identified in comparisons of sequences of CPI motifs across all protein families [Hernandez-Valladares, M., et al. (2010) Structural characterization of a capping protein interaction motif defines a family of actin filament regulators. , 497-503; Bruck, S., et al. (2006) Identification of a Novel Inhibitory Actin-capping Protein Binding Motif in CD2-associated Protein. , 19196-19203]. These biochemical differences may be important for conserved distinct functions of CPI-motif protein families in cells with respect to the regulation of CP activity and actin assembly near membranes.

摘要

肌动蛋白加帽蛋白 (CP) 的异二聚体由一组包含 CP 相互作用 (CPI) 基序的蛋白质调节。在 CPI 基序之外,这些蛋白质的序列是不相关且不同的。与其他 CPI 基序蛋白家族相比,给定蛋白家族内的 CPI 基序和周围序列是保守的。使用带有纯化蛋白的生化测定法,我们比较了来自不同蛋白家族的 CPI 基序肽 (a) 与 CP 结合的能力、(b) 变构抑制 CP 对珠状末端加帽的能力、以及 (c) 变构抑制 CP 与另一种 CP 调节剂 V-1 的相互作用的能力。我们发现不同 CPI 基序肽之间的效力有很大差异,并且不同的功能测定显示出不同的效力顺序。CPI 基序肽之间的这些生化差异可能反映了 CP 和 CPI 基序肽之间的相互作用,这些相互作用涉及氨基酸残基,这些残基是保守的,但不是最初在所有蛋白家族的 CPI 基序序列比较中确定的严格定义共识的一部分[Hernandez-Valladares, M., et al. (2010) 肌动蛋白加帽蛋白相互作用基序的结构特征定义了一组肌动蛋白丝调节剂。, 497-503;Bruck, S., et al. (2006) 鉴定 CD2 相关蛋白中的新型抑制性肌动蛋白加帽蛋白结合基序。, 19196-19203]。这些生化差异对于 CPI 基序蛋白家族在细胞中相对于 CP 活性和膜附近肌动蛋白组装的保守而独特的功能可能很重要。

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