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附睾成熟过程中与精子获能相关信号通路的发育。

Development of the signalling pathways associated with sperm capacitation during epididymal maturation.

作者信息

Baker Mark A, Lewis Beverley, Hetherington Louise, Aitken R John

机构信息

Discipline of Biological Sciences, School of Environmental and Life Sciences, University of Newcastle, Callaghan, NSW 2308, Australia.

出版信息

Mol Reprod Dev. 2003 Apr;64(4):446-57. doi: 10.1002/mrd.10255.

Abstract

As spermatozoa mature within the epididymis they acquire the potential for capacitation and ultimately fertilization. In biochemical terms, the former is reflected in the progressive activation of a signal transduction pathway characterized by cAMP-mediated induction of phosphotyrosine expression on the sperm tail. In this study, we have examined the cellular mechanisms controlling this maturational event. Caput epididymal spermatozoa exhibited tyrosine phosphorylation on the sperm head that was largely unresponsive to cAMP and not significantly impaired by removal of extracellular HCO(3) (-). In contrast, caudal epididymal spermatozoa exhibited low levels of phosphorylation on the sperm head, yet responded dramatically to cAMP by phosphorylating a new set of proteins on the sperm tail via mechanisms that were highly dependent on extracellular HCO(3) (-). The impact of extracellular HCO(3) (-) depletion on caudal cells was not associated with a significant change in the redox regulation of cAMP but could be fully reversed by buffering the intracellular pH with N-Tris[Hydroxymethyl]methyl-3-amino-propanesulfonic acid (TAPS). The pattern of tyrosine phosphorylation was also profoundly influenced by the presence or absence of added extracellular calcium. In the presence of this cation, only caudal spermatozoa could respond to increased extracellular cAMP with tyrosine phosphorylation of the sperm tail. However, in calcium-depleted medium, this difference completely disappeared. Under these conditions, caput and caudal spermatozoa were equally competent to exhibit phosphotyrosine expression on the sperm tail in response to cAMP. These results emphasize the pivotal role played by calcium and HCO(3) (-) in modulating the changes in tyrosine phosphorylation observed during epididymal maturation.

摘要

随着精子在附睾内成熟,它们获得了获能及最终受精的能力。从生化角度来看,前者表现为一条信号转导通路的逐步激活,其特征是cAMP介导精子尾部磷酸酪氨酸表达的诱导。在本研究中,我们研究了控制这一成熟事件的细胞机制。附睾头精子在精子头部表现出酪氨酸磷酸化,这在很大程度上对cAMP无反应,并且去除细胞外HCO(3)(-)后也没有明显受损。相比之下,附睾尾精子在精子头部表现出低水平的磷酸化,但通过高度依赖细胞外HCO(3)(-)的机制,使精子尾部一组新的蛋白质磷酸化,从而对cAMP产生显著反应。细胞外HCO(3)(-)耗尽对附睾尾细胞的影响与cAMP的氧化还原调节的显著变化无关,但用N-三[羟甲基]甲基-3-氨基丙烷磺酸(TAPS)缓冲细胞内pH值可使其完全逆转。酪氨酸磷酸化模式也受到添加或不添加细胞外钙的深刻影响。在这种阳离子存在的情况下,只有附睾尾精子能够通过精子尾部的酪氨酸磷酸化对细胞外cAMP增加做出反应。然而,在缺钙培养基中,这种差异完全消失。在这些条件下,附睾头和附睾尾精子在对cAMP的反应中,在精子尾部表现出磷酸酪氨酸表达的能力是相同的。这些结果强调了钙和HCO(3)(-)在调节附睾成熟过程中观察到的酪氨酸磷酸化变化中所起的关键作用。

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