Toxicants target cell junctions in the testis: Insights from the indazole-carboxylic acid model.

Spermatogenesis Pub Date : 2015-01-21 eCollection Date: 2014-05-01 DOI:10.4161/21565562.2014.981485
C Yan Cheng
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引用次数: 62

Abstract

There are numerous types of junctions in the seminiferous epithelium which are integrated with, and critically dependent on the Sertoli cell cytoskeleton. These include the basal tight junctions between Sertoli cells that form the main component of the blood-testis barrier, the basal ectoplasmic specializations (basal ES) and basal tubulobulbar complexes (basal TBC) between Sertoli cells; as well as apical ES and apical TBC between Sertoli cells and the developing spermatids that orchestrate spermiogenesis and spermiation. These junctions, namely TJ, ES, and TBC interact with actin microfilament-based cytoskeleton, which together with the desmosomal junctions that interact with the intermediate filament-based cytoskeleton plus the highly polarized microtubule-based cytoskeleton are working in concert to move spermatocytes and spermatids between the basal and luminal aspect of the seminiferous epithelium. In short, these various junctions are structurally complexed with the actin- and microtubule-based cytoskeleton or intermediate filaments of the Sertoli cell. Studies have shown toxicants (e.g., cadmium, bisphenol A (BPA), perfluorooctanesulfonate (PFOS), phthalates, and glycerol), and some male contraceptives under development (e.g., adjudin, gamendazole), exert their effects, at least in part, by targeting cell junctions in the testis. The disruption of Sertoli-Sertoli cell and Sertoli-germ cell junctions, results in the loss of germ cells from the seminiferous epithelium. Adjudin, a potential male contraceptive under investigation in our laboratory, produces loss of spermatids from the seminiferous tubules through disruption of the Sertoli cell spermatid junctions and disruption of the Sertoli cell cytoskeleton. The molecular and structural changes associated with adjudin administration are described, to provide an example of the profile of changes caused by disturbance of Sertoli-germ cell and also Sertoli cell-cell junctions.

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毒物靶细胞连接在睾丸:从吲哚-羧酸模型的见解。
在精原上皮中有许多类型的连接,这些连接与支持细胞骨架结合,并严重依赖于支持细胞骨架。这些包括构成血睾丸屏障主要成分的支持细胞之间的基础紧密连接,支持细胞之间的基础外质特化(basal ES)和基础管小球复合体(basal TBC);以及支持细胞和发育中的精子之间的顶端ES和顶端TBC,这些细胞协调精子的发生和受精。这些连接,即TJ、ES和TBC与基于肌动蛋白微丝的细胞骨架相互作用,它们与与基于中间丝的细胞骨架和高度极化的基于微管的细胞骨架相互作用的桥粒连接一起协同工作,使精母细胞和精子细胞在精原上皮的基底和腔面之间移动。简而言之,这些不同的连接在结构上与肌动蛋白和微管为基础的细胞骨架或支持细胞的中间丝复杂。研究表明,有毒物质(如镉、双酚A (BPA)、全氟辛烷磺酸(PFOS)、邻苯二甲酸盐和甘油)和一些正在开发的男性避孕药(如安非他明、甘美达唑),至少在一定程度上是通过靶向睾丸中的细胞连接来发挥作用的。支持-支持细胞和支持-生殖细胞连接的破坏导致生殖细胞从精原上皮中丢失。本实验室正在研究的一种潜在的男性避孕药裁决素,通过破坏支持细胞的精子细胞连接和破坏支持细胞的细胞骨架,从精管中产生精子的损失。描述了与裁决管理相关的分子和结构变化,以提供由支持生殖细胞和支持细胞-细胞连接的干扰引起的变化的一个例子。
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Computational characterization and integrative analysis of proteins involved in spermatogenesis Genetics of mammalian meiosis Roles of membrane and nuclear estrogen receptors in spermatogenesis Androgen regulation of spermatogenesis Cytoskeletons (F-actin) and spermatogenesis
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