首页> 外文期刊>Journal of Reproductive Immunology >Inhibition of 19S proteasomal regulatory complex subunit PSMD8 increases polyspermy during porcine fertilization in vitro.
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Inhibition of 19S proteasomal regulatory complex subunit PSMD8 increases polyspermy during porcine fertilization in vitro.

机译:体外猪受精过程中19S蛋白酶体调节复合物亚基PSMD8的抑制作用增加了多精子。

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摘要

The 26S proteoasome is a multi-subunit protease specific to ubiquitinated substrate proteins. It is composed of a 20S proteasomal core with substrate degradation activity, and a 19S regulatory complex that acts in substrate recognition, deubiquitination, priming and transport to the 20S core. Inhibition of proteolytic activities associated with the sperm acrosome-borne 20S core prevents fertilization in mammals, ascidians and echinoderms. Less is known about the function of the proteasomal 19S complex during fertilization. The present study examined the role of PSMD8, an essential non-ATPase subunit of the 19S complex, in sperm-ZP penetration during porcine fertilization in vitro (IVF). Immunofluorescence localized PSMD8 to the outer acrosomal membrane, acrosomal matrix and the inner acrosomal membrane. Colloidal gold transmission electron microscopy detected PSMD8 on the surface of vesicles in the acrosomal shroud, formed as a result of zona pellucida-induced acrosomal exocytosis. Contrary to the inhibition of fertilization by blocking of the 20S core activities, fertilization and polyspermy rates were increased by adding anti-PSMD8 antibody to fertilization medium. This observation is consistent with a possible role of PSMD8 in substrate deubiquitination, a process which when blocked, may actually accelerate substrate proteolysis by the 26S proteasome. Subunit PSMD8 co-immunoprecipitated with acrosomal surface-associated spermadhesin AQN1. This association indicates that the sperm acrosome-borne proteasomes become exposed onto the sperm surface following the acrosomal exocytosis. Since immunological blocking of subunit PSMD8 increases the rate of polyspermy during porcine fertilization, the activity of the 19S complex may be a rate-limiting factor contributing to anti-polyspermy defense during porcine fertilization.
机译:26S蛋白囊泡是一种泛素化底物蛋白特异的多亚基蛋白酶。它由具有底物降解活性的20S蛋白酶体核心和在底物识别,去泛素化,引发和转运至20S核心中起作用的19S调节复合物组成。抑制与精子顶体携带的20S核心相关的蛋白水解活性可防止哺乳动物,海鞘和棘皮动物受精。对蛋白酶体19S复合物在受精过程中的功能了解甚少。本研究检查了PSMD8(19S复合物的必需非ATPase亚基)在体外猪受精(IVF)过程中对精子ZP渗透的作用。免疫荧光使PSMD8定位于顶体外膜,顶体基质和顶体内膜。胶体金透射电子显微镜检测到顶体覆盖物中囊泡表面上的PSMD8,这是透明带引起的顶体胞吐作用的结果。与通过阻断20S核心活性而抑制受精相反,向受精培养基中添加抗PSMD8抗体可提高受精率和多精子率。该观察结果与PSMD8在底物去泛素化中的可能作用是一致的,该过程在被阻断时实际上可以加速26S蛋白酶体的底物蛋白水解。亚基PSMD8与顶体表面相关精子粘附素AQN1共免疫沉淀。这种联系表明,在顶体胞吐作用之后,精子顶体携带的蛋白酶体暴露于精子表面。由于亚基PSMD8的免疫阻断增加了猪受精过程中多精子的比率,因此19S复合物的活性可能是限速因素,有助于猪受精过程中的抗多精子防御。

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