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豚鼠精子发生过程中特异性结构域顶体基质蛋白AM50的分选

Sorting of the domain-specific acrosomal matrix protein AM50 during spermiogenesis in the guinea pig.

作者信息

Westbrook-Case V A, Winfrey V P, Olson G E

机构信息

Department of Cell Biology, Vanderbilt University, Nashville, Tennessee 37232.

出版信息

Dev Biol. 1995 Jan;167(1):338-49. doi: 10.1006/dbio.1995.1028.

Abstract

We previously identified an insoluble 50-kDa acrosomal matrix protein (AM50) localized to the ventral region of the guinea pig sperm apical segment. AM50 is converted to a 42-kDa polypeptide and released during matrix dispersion in acrosome-reacting sperm. This study examines the sorting pathways and assembly processes which generate the domain-specific distribution of AM50 in the acrosome. AM50 was expressed during early acrosome development and localized to the matrix of proacrosomal granules and the acrosomal vesicle. Initial sorting of AM50 occurred in Golgi phase spermatids, where it became concentrated in the matrix surrounding the acrosomal granule. AM50 remained restricted to the apical segment of acrosome phase spermatids and was finally sorted to the ventral matrix of the apical segment in maturation phase spermatids. By reducing SDS-PAGE testicular AM50 exhibited a slightly higher M(r) of 52 kDa than the 50-kDa form of cauda epididymal spermatozoa. Nonreducing SDS-PAGE demonstrated that testicular and epididymal AM50 were assembled into homomeric complexes of 480 and 450 kDa respectively. Cauda epididymal sperm apical segments contained a second disulfide-cross-linked homomeric complex of 520 kDa composed of a 68-kDa subunit. These studies indicate that AM50 is first assembled into a disulfide-cross-linked complex and subsequently processed into mature AM50. These data also suggest that disulfide-linked complexes of different structural proteins may assemble into distinct acrosomal matrix compartments.

摘要

我们之前鉴定出一种不溶性的50 kDa顶体基质蛋白(AM50),定位于豚鼠精子顶段的腹侧区域。在顶体反应的精子中,AM50在顶体基质分散过程中转化为42 kDa的多肽并释放出来。本研究考察了产生AM50在顶体中区域特异性分布的分选途径和组装过程。AM50在顶体早期发育过程中表达,定位于前顶体颗粒和顶体小泡的基质中。AM50的初始分选发生在高尔基体期精子细胞中,在那里它集中在围绕顶体颗粒的基质中。AM50仍局限于顶体期精子细胞的顶段,最终在成熟精子细胞中被分选到顶段的腹侧基质中。通过SDS-PAGE还原,睾丸中的AM50显示出略高于52 kDa的分子量,而附睾尾精子的分子量为50 kDa。非还原SDS-PAGE表明,睾丸和附睾中的AM50分别组装成480 kDa和450 kDa的同聚体复合物。附睾尾精子顶段含有由68 kDa亚基组成的第二个520 kDa的二硫键交联同聚体复合物。这些研究表明,AM50首先组装成二硫键交联复合物,随后加工成成熟的AM50。这些数据还表明,不同结构蛋白的二硫键连接复合物可能组装成不同的顶体基质区室。

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