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Na,K-ATPase alpha4 同工酶的活性对于维持精子运动性的膜电位、细胞内 Ca2+ 和 pH 非常重要。

Activity of the Na,K-ATPase alpha4 isoform is important for membrane potential, intracellular Ca2+, and pH to maintain motility in rat spermatozoa.

机构信息

Department of Molecular and Integrative Physiology, University of Kansas Medical Center, 3901 Rainbow Boulevard, Kansas City, Kansas 66160, USA.

出版信息

Reproduction. 2010 May;139(5):835-45. doi: 10.1530/REP-09-0495. Epub 2010 Feb 23.

Abstract

While the function of the ubiquitous Na,K-ATPase alpha1 subunit has been well documented, the role of the sperm-specific alpha4 isoform of this ion transporter is less known. We have explored the importance of alpha4 in rat sperm physiology by taking advantage of the high sensitivity of this isoform for the inhibitor ouabain. Using concentrations that selectively block alpha4 activity, we found ouabain to reduce not only sperm total motility, but also multiple parameters of sperm movement, including progressive motility, straight line, curvilinear, and average path velocities, lateral head displacement, beat cross frequency, and linearity. According to a direct role of alpha4 in Na(+) transport, ouabain inhibition of alpha4 increased Na(+) in the male gametes. In addition, interference of alpha4 activity with ouabain produced cell membrane depolarization, diminished pH, and increased Ca(2)(+) in spermatozoa. Inhibition of alpha4 was sufficient to cause all these effects and additional blockage of alpha1, the other Na,K-ATPase alpha isoform expressed in sperm, and higher doses of ouabain did not result in further changes in the cell parameters studied. These results show that alpha4 is the Na,K-ATPase isoform primarily involved in controlling the transmembrane Na(+) gradient in sperm, and that alpha4 activity is necessary for maintaining membrane potential, Ca(2)(+), and H(+) in the cells. The high dependence of sperm motility on membrane excitability, Ca(2)(+), and acid-base balance suggests that their regulation is the mechanism by which alpha4 maintains motility of the male gametes.

摘要

虽然普遍存在的 Na,K-ATPase alpha1 亚基的功能已经得到很好的证明,但这种离子转运体的精子特异性 alpha4 同工型的作用知之甚少。我们利用这种同工型对抑制剂哇巴因的高敏感性,探索了 alpha4 在大鼠精子生理学中的重要性。使用选择性阻断 alpha4 活性的浓度,我们发现哇巴因不仅降低了精子的总活力,还降低了精子运动的多个参数,包括前向运动、直线、曲线和平均路径速度、侧向头部位移、鞭打交叉频率和直线性。根据 alpha4 在 Na+转运中的直接作用,哇巴因抑制 alpha4 增加了雄性配子中的Na+。此外,alpha4 活性与哇巴因的干扰导致细胞膜去极化、pH 值降低和精子中的Ca2+增加。alpha4 的抑制足以引起所有这些效应,并且阻断 alpha1(在精子中表达的另一种 Na,K-ATPase alpha 同工型)的进一步干扰会导致所研究的细胞参数没有进一步变化。这些结果表明,alpha4 是主要参与控制精子跨膜 Na+梯度的 Na,K-ATPase 同工型,并且 alpha4 活性对于维持膜电位、Ca2+和细胞中的H+是必要的。精子活力对膜兴奋性、Ca2+和酸碱平衡的高度依赖性表明,它们的调节是 alpha4 维持雄性配子活力的机制。

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