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精子获能的分子机制:孕酮诱导的继发性钙振荡反映了获能状态的达成。

Molecular mechanisms of sperm capacitation: progesterone-induced secondary calcium oscillations reflect the attainment of a capacitated state.

作者信息

Aitken R J, McLaughlin E A

机构信息

RC Centre of Excellence in Biotechnology and Development, Discipline of Biological Sciences, University of Newcastle, Callaghan, NSW 2708, Australia.

出版信息

Soc Reprod Fertil Suppl. 2007;63:273-93.

Abstract

Progesterone has an extragenomic action on human spermatozoa characterised by the rapid induction of a calcium transient followed by a plateau phase during which [Ca2+], remains significantly above baseline. By imaging the calcium responses generated in individual cells, we have demonstrated that during this plateau phase, spermatozoa exhibit a series of asynchronous secondary calcium oscillations. The incidence of such oscillations was dependent upon sperm capacitation and showed significant inter-individual variation. The oscillations were dependent upon the influx of extracellular calcium via mechanisms that were insensitive to inhibitors of L-type voltage operated calcium channels (nifedipine, verapamil, diltiazem), G-proteins (pertussis toxin) or the GABA (A) receptor (bicuculline). However, treatment with an inhibitor of the GABA-associated chloride channel (picrotoxin) significantly suppressed the incidence of secondary calcium oscillations in pentoxifylline-treated cells, as did two inhibitors of T-type calcium channels (pimozide and amiloride). We hypothesise that the sub-population of spermatozoa exhibiting secondary calcium oscillations are characterised by a hyperpolarized plasma membrane that sets T-type channels in a closed but activation-competent state. The secondary calcium oscillations created via these channels do not induce acrosomal exocytosis per se but may prime the cells so that this event is rapidly triggered when the spermatozoa make contact with the zona pellucida.

摘要

孕酮对人类精子具有一种基因组外作用,其特征是迅速诱导钙瞬变,随后进入一个平台期,在此期间细胞内钙离子浓度([Ca2+]i)仍显著高于基线水平。通过对单个细胞产生的钙反应进行成像,我们已经证明,在这个平台期,精子会表现出一系列异步的继发性钙振荡。这种振荡的发生率取决于精子的获能情况,并且在个体之间存在显著差异。这些振荡依赖于细胞外钙的内流,其机制对L型电压门控钙通道抑制剂(硝苯地平、维拉帕米、地尔硫䓬)、G蛋白(百日咳毒素)或GABA(A)受体抑制剂(荷包牡丹碱)不敏感。然而,用GABA相关氯通道抑制剂(印防己毒素)处理,可显著抑制己酮可可碱处理细胞中继发性钙振荡的发生率,两种T型钙通道抑制剂(匹莫齐特和阿米洛利)也有同样的效果。我们推测,表现出继发性钙振荡的精子亚群的特征是质膜超极化,这使得T型通道处于关闭但具有激活能力的状态。通过这些通道产生的继发性钙振荡本身不会诱导顶体胞吐,但可能使细胞致敏,以便当精子与透明带接触时能迅速触发这一事件。

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