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发现并描述磷酸烯醇式丙酮酸载体/SIMP/病毒蛋白超家族。

Discovery and Characterization of the Phospholemman/SIMP/Viroporin Superfamily.

机构信息

Department of Molecular Biology, Division of Biological Sciences, University of California San Diego, La Jolla, California, USA.

出版信息

Microb Physiol. 2022;32(3-4):83-94. doi: 10.1159/000521947. Epub 2022 Feb 11.

Abstract

Using bioinformatic approaches, we present evidence of distant relatedness among the Ephemerovirus Viroporin family, the Rhabdoviridae Putative Viroporin U5 family, the Phospholemman family, and the Small Integral Membrane Protein family. Our approach is based on the transitivity property of homology complemented with five validation criteria: (1) significant sequence similarity and alignment coverage, (2) compatibility of topology of transmembrane segments, (3) overlap of hydropathy profiles, (4) conservation of protein domains, and (5) conservation of sequence motifs. Our results indicate that Pfam protein domains PF02038 and PF15831 can be found in or projected onto members of all four families. In addition, we identified a 26-residue motif conserved across the superfamily. This motif is characterized by hydrophobic residues that help anchor the protein to the membrane and charged residues that constitute phosphorylation sites. In addition, all members of the four families with annotated function are either responsible for or affect the transport of ions into and/or out of the cell. Taken together, these results justify the creation of the novel Phospholemman/SIMP/Viroporin superfamily. Given that transport proteins can be found not just in cells, but also in viruses, the ability to relate viroporin protein families with their eukaryotic and bacterial counterparts is an important development in this superfamily.

摘要

利用生物信息学方法,我们证明了弹状病毒属的 Viroporin 家族、副黏病毒科的推定 Viroporin U5 家族、磷酸鞘氨醇家族和小整合膜蛋白家族之间存在远缘关系。我们的方法基于同源性的传递性,并辅以五个验证标准:(1)显著的序列相似性和对齐覆盖率,(2)跨膜片段拓扑的兼容性,(3)疏水性轮廓的重叠,(4)蛋白质结构域的保守性,以及(5)序列基序的保守性。我们的结果表明,Pfam 蛋白结构域 PF02038 和 PF15831 可以在四个家族的成员中找到或投影到这些成员中。此外,我们还鉴定了一个横跨超家族保守的 26 个残基基序。这个基序的特点是疏水残基,这些残基有助于将蛋白质锚定在膜上,而带电荷的残基则构成磷酸化位点。此外,所有具有注释功能的四个家族的成员都负责或影响离子进出细胞的运输。综上所述,这些结果证明了创建新型磷酸鞘氨醇/SIMP/Viroporin 超家族的合理性。鉴于运输蛋白不仅存在于细胞中,也存在于病毒中,因此将 Viroporin 蛋白家族与其真核和细菌对应物相关联的能力是这个超家族的一个重要发展。

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