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人类精子上的相互作用蛋白:精囊蛋白 I 与 EPPIN 结合的适应性进化。

Interacting proteins on human spermatozoa: adaptive evolution of the binding of semenogelin I to EPPIN.

机构信息

Department of Cell Biology & Physiology, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, United States of America.

出版信息

PLoS One. 2013 Dec 2;8(12):e82014. doi: 10.1371/journal.pone.0082014. eCollection 2013.

DOI:10.1371/journal.pone.0082014
PMID:24312623
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3846889/
Abstract

Semenogelin I (SEMG1) is found in human semen coagulum and on the surface of spermatozoa bound to EPPIN. The physiological significance of the SEMG1/EPPIN interaction on the surface of spermatozoa is its capacity to modulate sperm progressive motility. The present study investigates the hypothesis that the interacting surface of SEMG1 and EPPIN co-evolved within the Hominoidea time scale, as a result of adaptive pressures applied by their roles in sperm protection and reproductive fitness. Our results indicate that some amino acid residues of SEMG1 and EPPIN possess a remarkable deficiency of variation among hominoid primates. We observe a distinct residue change unique to humans within the EPPIN sequence containing a SEMG1 interacting surface, namely His92. In addition, Bayes Empirical Bayes analysis for positive selection indicates that the SEMG1 Cys239 residue underwent positive selection in humans, probably as a consequence of its role in increasing the binding affinity of these interacting proteins. We confirm the critical role of Cys239 residue for SEMG1 binding to EPPIN and inhibition of sperm motility by showing that recombinant SEMG1 mutants in which Cys239 residue was changed to glycine, aspartic acid, histidine, serine or arginine have reduced capacity to interact to EPPIN and to inhibit human sperm motility in vitro. In conclusion, our results indicate that EPPIN and SEMG1 rapidly co-evolved in primates due to their critical role in the modulation of sperm motility in the semen coagulum, providing unique insights into the molecular co-evolution of sperm surface interacting proteins.

摘要

精球蛋白 I(SEMG1)存在于人类精液凝块中,并与精子表面的 EPPIN 结合。SEMG1/EPPIN 相互作用在精子表面的生理意义在于其调节精子前向运动的能力。本研究假设 SEMG1 和 EPPIN 的相互作用表面在 Homoidea 时间尺度内共同进化,这是它们在精子保护和生殖适应性方面的作用所施加的适应性压力的结果。我们的结果表明,SEMG1 和 EPPIN 的一些氨基酸残基在灵长类动物中存在明显的变异不足。我们观察到 EPPIN 序列中存在一个独特的人类残基变化,其中包含一个 SEMG1 相互作用表面,即 His92。此外,正选择的贝叶斯经验贝叶斯分析表明,SEMG1 的 Cys239 残基在人类中经历了正选择,可能是由于其增加这些相互作用蛋白结合亲和力的作用。我们通过显示 Cys239 残基突变为甘氨酸、天冬氨酸、组氨酸、丝氨酸或精氨酸的重组 SEMG1 突变体与 EPPIN 的结合能力降低,并且抑制人精子体外运动,从而证实了 Cys239 残基对 SEMG1 与 EPPIN 结合和抑制人精子运动的关键作用。总之,我们的研究结果表明,EPPIN 和 SEMG1 在灵长类动物中快速共同进化,这是因为它们在精液凝块中调节精子运动的关键作用,为精子表面相互作用蛋白的分子共同进化提供了独特的见解。

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Mol Biol Evol. 2013 Apr;30(4):938-50. doi: 10.1093/molbev/mss329. Epub 2013 Jan 4.
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Characterization of EPPIN's semenogelin I binding site: a contraceptive drug target.EPPIN 精液蛋白 I 结合位点的特性:一种避孕药物靶点。
Biol Reprod. 2012 Sep 7;87(3):56. doi: 10.1095/biolreprod.112.101832. Print 2012 Sep.
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Loss of calcium in human spermatozoa via EPPIN, the semenogelin receptor.人类精子中钙通过 EPPIN(精液蛋白受体)丢失。
解脲脲原体诱导多形核弹性蛋白酶改变精液特性并降低精子活力:一项前瞻性观察性研究。
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Human Semenogelin 1 Promotes Sperm Survival in the Mouse Female Reproductive Tract.人精液蛋白 1 促进小鼠雌性生殖道内精子存活。
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Binding interactions of epididymal protease inhibitor and semenogelin-1: a homology modeling, docking and molecular dynamics simulation study.附睾蛋白酶抑制剂与精液凝胶蛋白-1的结合相互作用:同源建模、对接及分子动力学模拟研究
PeerJ. 2019 Aug 5;7:e7329. doi: 10.7717/peerj.7329. eCollection 2019.
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Recent Developments in Male Contraception.男性避孕的最新进展。
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The Expressional Pattern of Epididymal Protease Inhibitor (EPPIN) in the Male Syrian Hamsters.雄性叙利亚仓鼠中附睾蛋白酶抑制剂(EPPIN)的表达模式
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10
Inhibition of human sperm motility by contraceptive anti-eppin antibodies from infertile male monkeys: effect on cyclic adenosine monophosphate.来自不育雄猴的避孕抗附睾分泌蛋白Eppin抗体对人类精子活力的抑制作用:对环磷酸腺苷的影响
Biol Reprod. 2009 Feb;80(2):279-85. doi: 10.1095/biolreprod.108.072942. Epub 2008 Oct 22.