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结构洞察秀丽隐杆线虫 fidgetin 样蛋白 1(FIGL-1)的 AAA 结构域异常强的 ATP 酶活性。

Structural insights into the unusually strong ATPase activity of the AAA domain of the Caenorhabditis elegans fidgetin-like 1 (FIGL-1) protein.

机构信息

From the Institute of Protein Research, Tongji University, Shanghai 200092 and.

出版信息

J Biol Chem. 2013 Oct 11;288(41):29305-12. doi: 10.1074/jbc.M113.502559. Epub 2013 Aug 26.

Abstract

The FIGL-1 (fidgetin like-1) protein is a homolog of fidgetin, a protein whose mutation leads to multiple developmental defects. The FIGL-1 protein contains an AAA (ATPase associated with various activities) domain and belongs to the AAA superfamily. However, the biological functions and developmental implications of this protein remain unknown. Here, we show that the AAA domain of the Caenorhabditis elegans FIGL-1 protein (CeFIGL-1-AAA), in clear contrast to homologous AAA domains, has an unusually high ATPase activity and forms a hexamer in solution. By determining the crystal structure of CeFIGL-1-AAA, we found that the loop linking helices α9 and α10 folds into the short helix α9a, which has an acidic surface and interacts with a positively charged surface of the neighboring subunit. Disruption of this charge interaction by mutagenesis diminishes both the ATPase activity and oligomerization capacity of the protein. Interestingly, the acidic residues in helix α9a of CeFIGL-1-AAA are not conserved in other homologous AAA domains that have relatively low ATPase activities. These results demonstrate that the sequence of CeFIGL-1-AAA has adapted to establish an intersubunit charge interaction, which contributes to its strong oligomerization and ATPase activity. These unique properties of CeFIGL-1-AAA distinguish it from other homologous proteins, suggesting that CeFIGL-1 may have a distinct biological function.

摘要

FIGL-1(烦躁不安样蛋白 1)蛋白是 fidgetin 的同源物,其突变会导致多种发育缺陷。FIGL-1 蛋白含有一个 AAA(与各种活性相关的 ATP 酶)结构域,属于 AAA 超家族。然而,该蛋白的生物学功能和发育意义尚不清楚。在这里,我们表明,Caenorhabditis elegans FIGL-1 蛋白(CeFIGL-1-AAA)的 AAA 结构域与同源的 AAA 结构域明显不同,具有异常高的 ATP 酶活性,并在溶液中形成六聚体。通过确定 CeFIGL-1-AAA 的晶体结构,我们发现连接α9 和α10 螺旋的环折叠成短的α9a 螺旋,该螺旋具有酸性表面,并与相邻亚基的带正电荷表面相互作用。通过突变破坏这种电荷相互作用会降低蛋白的 ATP 酶活性和寡聚化能力。有趣的是,CeFIGL-1-AAA 的α9a 螺旋中的酸性残基在其他具有相对较低 ATP 酶活性的同源 AAA 结构域中没有保守。这些结果表明,CeFIGL-1-AAA 的序列已经适应于建立亚基间的电荷相互作用,这有助于其强烈的寡聚化和 ATP 酶活性。CeFIGL-1-AAA 的这些独特性质使其与其他同源蛋白区分开来,表明 CeFIGL-1 可能具有独特的生物学功能。

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