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肌动蛋白单体结合蛋白与Srv2/CAP相互作用的机制及生物学作用

Mechanism and biological role of profilin-Srv2/CAP interaction.

作者信息

Bertling Enni, Quintero-Monzon Omar, Mattila Pieta K, Goode Bruce L, Lappalainen Pekka

机构信息

Institute of Biotechnology, University of Helsinki, 00014 Helsinki, Finland.

出版信息

J Cell Sci. 2007 Apr 1;120(Pt 7):1225-34. doi: 10.1242/jcs.000158.

DOI:10.1242/jcs.000158
PMID:17376963
Abstract

Profilin and cyclase-associated protein (CAP, known in yeast as Srv2) are ubiquitous and abundant actin monomer-binding proteins. Profilin catalyses the nucleotide exchange on actin monomers and promotes their addition to filament barbed ends. Srv2/CAP recycles newly depolymerized actin monomers from ADF/cofilin for subsequent rounds of polymerization. Srv2/CAP also harbors two proline-rich motifs and has been suggested to interact with profilin. However, the mechanism and biological role of the possible profilin-Srv2/CAP interaction has not been investigated. Here, we show that Saccharomyces cerevisiae Srv2 and profilin interact directly (K(D) approximately 1.3 microM) and demonstrate that a specific proline-rich motif in Srv2 mediates this interaction in vitro and in vivo. ADP-actin monomers and profilin do not interfere with each other's binding to Srv2, suggesting that these three proteins can form a ternary complex. Genetic and cell biological analyses on an Srv2 allele (srv2-201) defective in binding profilin reveals that a direct interaction with profilin is not essential for Srv2 cellular function. However, srv2-201 causes a moderate increase in cell size and partially suppresses the cell growth and actin organization defects of an actin binding mutant profilin (pfy1-4). Together these data suggest that Srv2 is an important physiological interaction partner of profilin.

摘要

肌动蛋白单体结合蛋白(肌动蛋白单体结合蛋白和环化酶相关蛋白(CAP,在酵母中称为Srv2))广泛存在且含量丰富。肌动蛋白单体结合蛋白催化肌动蛋白单体上的核苷酸交换,并促进其添加到细丝的带刺末端。Srv2/CAP从ADF/丝切蛋白回收新解聚的肌动蛋白单体,用于后续的聚合反应。Srv2/CAP还含有两个富含脯氨酸的基序,并被认为与肌动蛋白单体结合蛋白相互作用。然而,肌动蛋白单体结合蛋白-Srv2/CAP可能相互作用的机制和生物学作用尚未得到研究。在这里,我们表明酿酒酵母Srv2和肌动蛋白单体结合蛋白直接相互作用(K(D)约为1.3 microM),并证明Srv2中一个特定的富含脯氨酸的基序在体外和体内介导这种相互作用。ADP-肌动蛋白单体和肌动蛋白单体结合蛋白不会相互干扰与Srv2的结合,这表明这三种蛋白质可以形成三元复合物。对与肌动蛋白单体结合蛋白结合缺陷的Srv2等位基因(srv2-201)进行的遗传和细胞生物学分析表明,与肌动蛋白单体结合蛋白的直接相互作用对Srv2的细胞功能不是必需的。然而,srv2-201会导致细胞大小适度增加,并部分抑制肌动蛋白结合突变体肌动蛋白单体结合蛋白(pfy1-4)的细胞生长和肌动蛋白组织缺陷。这些数据共同表明Srv2是肌动蛋白单体结合蛋白的重要生理相互作用伙伴。

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