首页> 外文期刊>Cell and Tissue Research >Interference with the 19S proteasomal regulatory complex subunit PSMD4 on the sperm surface inhibits sperm-zona pellucida penetration during porcine fertilization.
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Interference with the 19S proteasomal regulatory complex subunit PSMD4 on the sperm surface inhibits sperm-zona pellucida penetration during porcine fertilization.

机译:精子表面干扰19S蛋白酶体调节复合物亚基PSMD4会抑制猪受精过程中的精子-透明带穿透。

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摘要

Proteolysis of ubiquitinated sperm and oocyte proteins by the 26S proteasome is necessary for the success of mammalian fertilization, including but not limited to acrosomal exocytosis and sperm-zona pellucida (ZP) penetration. The present study examined the role of PSMD4, an essential non-ATPase subunit of the proteasomal 19S regulatory complex responsible for proteasome-substrate recognition, in sperm-ZP penetration during porcine fertilization in vitro (IVF). Porcine sperm-ZP penetration, but not sperm-ZP binding, was blocked in the presence of a monoclonal anti-PSMD4 antibody during IVF. Inclusion in the fertilization medium of mutant ubiquitins (Ub+1 and Ub5+1), which are refractory to processing by the 19S regulatory complex and associated with Alzheimer's disease, also inhibited fertilization. This observation suggested that subunit PSMD4 is exposed on the sperm acrosomal surface, a notion that was further supported by the binding of non-cell permeant, biotinylated proteasomal inhibitor ZL3VS to the sperm acrosome. Immunofluorescence localized PSMD4 in the sperm acrosome. Immunoprecipitation and proteomic analysis revealed that PSMD4 co-precipitated with porcine sperm-associated acrosin inhibitor (AI). Ubiquitinated species of AI were isolated from boar sperm extracts by affinity purification of ubiquitinated proteins using the recombinant UBA domain of p62 protein. Some proteasomes appeared to be anchored to the sperm head inner acrosomal membrane, as documented by co-fractionation studies. In conclusion, the 19S regulatory complex subunit PSMD4 is involved in the sperm-ZP penetration during fertilization. The recognition of substrates on the ZP by the 19S proteasomal regulatory complex is essential for the success of porcine/mammalian fertilization in vitro.
机译:26S蛋白酶体对遍在蛋白化的精子和卵母蛋白进行蛋白水解对于哺乳动物受精的成功是必要的,包括但不限于顶体胞吐作用和透皮精子(ZP)渗透。本研究检查了PSMD4,它是蛋白酶体19S调控复合体的重要非ATPase亚基,负责蛋白酶体-底物的识别,在猪体外受精(IVF)过程中对精子ZP的渗透作用。在IVF期间,在存在单克隆抗PSMD4抗体的情况下,猪的精子-ZP穿透力被阻止,但精子-ZP的结合未被阻断。突变体遍在蛋白(Ub + 1和Ub5 + 1)在受精培养基中的加入对19S调控复合物的加工是难治的,并且与阿尔茨海默氏病有关,也抑制了受精。该观察结果表明亚基PSMD4暴露于精子顶体表面,非细胞渗透性生物素化蛋白酶体抑制剂ZL3VS与精子顶体的结合进一步支持了这一观念。免疫荧光将PSMD4定位在精子顶体中。免疫沉淀和蛋白质组学分析表明,PSMD4与猪精子相关的丙烯醛抑制剂(AI)共沉淀。通过使用p62蛋白的重组UBA域亲和纯化泛素化的蛋白质,从公猪精子提取物中分离出泛素化的AI。共分离研究表明,一些蛋白酶体似乎锚定在精子顶顶体内膜上。总之,受精过程中19S调控复合物亚基PSMD4参与了精子ZP的渗透。 19S蛋白酶体调控复合物识别ZP上的底物对于猪/哺乳动物体外受精的成功至关重要。

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