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人类精子中酪氨酸磷酸化的氧化还原调节及其在人类精子功能控制中的作用。

Redox regulation of tyrosine phosphorylation in human spermatozoa and its role in the control of human sperm function.

作者信息

Aitken R J, Paterson M, Fisher H, Buckingham D W, van Duin M

机构信息

MRC Reproductive Biology Unit, Edinburgh, Scotland.

出版信息

J Cell Sci. 1995 May;108 ( Pt 5):2017-25. doi: 10.1242/jcs.108.5.2017.

DOI:10.1242/jcs.108.5.2017
PMID:7544800
Abstract

The redox status of human spermatozoa was found to have a profound influence on the fertilizing potential of these cells in association with qualitative and quantitative changes in the patterns of tyrosine phosphorylation. In general, oxidizing conditions enhanced tyrosine phosphorylation and stimulated sperm function, whereas reducing conditions had the opposite effect. Unstimulated human spermatozoa exhibited low levels of spontaneous acrosomal exocytosis and sperm-oocyte fusion and minimal reactive oxygen species generation, while phosphotyrosine expression was largely confined to a single protein of 116 kDa. However, if the spermatozoa were exposed to oxidizing conditions through the addition of exogenous H2O2, or the stimulation of endogenous NADPH-dependent reactive oxygen species generation, then a dramatic increase in tyrosine phosphorylation was observed (major phosphotyrosyl bands at 222 kDa, 200 kDa, 159 kDa, 133 kDa, 116 kDa and 82 kDa) in concert with the functional activation of the spermatozoa. A causal association between reactive oxygen species generation, tyrosine phosphorylation and sperm function was indicated by studies with the ionophore, A23187, which induced high rates of spermoocyte fusion together with enhanced rates of reactive oxygen species production and the increased expression of phosphotyrosyl proteins. This functional response to A23187 could be abrogated, without any concomitant change in sperm motility or viability, by using membrane permeant thiols or catalase to suppress the reactive oxygen species-induced increase in phosphotyrosine expression. The fact that the biological responses of human spermatozoa to biological agonists (recombinant human ZP3 and progesterone) could also be inhibited by catalase indicated the general relevance of these findings.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

研究发现,人类精子的氧化还原状态与酪氨酸磷酸化模式的定性和定量变化相关,对这些细胞的受精潜力具有深远影响。一般来说,氧化条件会增强酪氨酸磷酸化并刺激精子功能,而还原条件则产生相反的效果。未受刺激的人类精子表现出低水平的自发顶体胞吐和精子-卵母细胞融合,活性氧生成极少,而磷酸酪氨酸表达主要局限于一种116 kDa的单一蛋白质。然而,如果通过添加外源性H2O2或刺激内源性NADPH依赖性活性氧生成使精子暴露于氧化条件下,那么会观察到酪氨酸磷酸化显著增加(主要磷酸酪氨酸条带位于222 kDa、200 kDa、159 kDa、133 kDa、116 kDa和82 kDa),同时精子功能被激活。用离子载体A23187进行的研究表明活性氧生成、酪氨酸磷酸化与精子功能之间存在因果关系,A23187诱导了高比率的精子-卵母细胞融合以及活性氧生成率的提高和磷酸酪氨酸蛋白表达的增加。通过使用膜渗透性硫醇或过氧化氢酶抑制活性氧诱导的磷酸酪氨酸表达增加,这种对A23187的功能反应可以被消除,而精子活力或生存能力没有任何相应变化。过氧化氢酶也能抑制人类精子对生物激动剂(重组人ZP3和孕酮)的生物学反应,这一事实表明了这些发现的普遍相关性。(摘要截短至250字)

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