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首页> 外文期刊>American Journal of Physiology >Regulation of the blood-testis barrier by coxsackievirus and adenovirus receptor
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Regulation of the blood-testis barrier by coxsackievirus and adenovirus receptor

机译:柯萨奇病毒和腺病毒受体调节血液-睾丸屏障

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The blood-testis barrier (BTB) divides the seminiferous epithelium into the basal and the adluminal compartment. It restricts paracellular diffusion of molecules between Sertoli cells, confers cell polarity, and creates a unique microenvironment in the adluminal compartment for spermatid development. However, it undergoes restructuring during the epithelial cycle so that preleptotene spermatocytes differentiated from type B spermatogonia residing in the basal compartment can traverse the BTB at stage VIII of the cycle, while the immunological barrier is maintained. Herein, coxsackievirus and adenovirus receptor (CAR), a tight junction (TJ) integral membrane protein in the testis and multiple epithelia and endothelia, was found to act as a regulatory protein at the BTB, besides serving as a structural adhesion protein. RNAi-mediated knockdown of CAR in a Sertoli cell epithelium with an established TJ-permeability barrier that mimicked the BTB in vivo resulted in a disruption of the TJ barrier and an increase in endocytosis of the TJ-protein occludin. Furthermore, such an enhancement in occludin endocytosis was accompanied by a downregulation of Thr-phosphor-ylation in occludin and an increase in the association of endocytosed occludin with early endosome antigen-1. These findings were confirmed by overexpressing CAR in Sertoli cells, which was found to "tighten" the Sertoli cell TJ barrier, promoting BTB function. These findings support the emerging concept that CAR is not only a structural protein, it is involved in conferring the phosphorylation status of other adhesion proteins at the BTB (e.g., occludin) possibly mediated via its structural interactions with nonreceptor protein ki-nases, thereby modulating endocytic vesicle-mediated protein trafficking.
机译:血液-睾丸屏障(BTB)将生精上皮分为基底和肾上腺区室。它限制了支持细胞之间分子的细胞旁扩散,赋予细胞极性,并在肾小管腔内为精子细胞的发育创造了独特的微环境。但是,它在上皮周期中进行重组,因此与位于基底区室的B型精原细胞分化的前瘦素精细胞可以在周期的VIII期穿越BTB,同时保持了免疫屏障。在本文中,发现柯萨奇病毒和腺病毒受体(CAR)是睾丸以及多个上皮和内皮中的紧密连接(TJ)整合膜蛋白,除了充当结构粘附蛋白外,还作为BTB的调节蛋白。 RNAi介导的Sertoli细胞上皮中的CAR敲除具有已建立的TJ渗透性屏障,在体内模仿了BTB,导致TJ屏障的破坏和TJ蛋白封端蛋白的内吞作用增加。此外,这种闭合蛋白内吞作用的增强伴随着闭合蛋白中Thr-磷酸化的下调以及内吞的闭合蛋白与早期内体抗原-1的结合增加。这些发现被Sertoli细胞中过表达CAR所证实,后者被发现“收紧”了Sertoli细胞的TJ屏障,促进了BTB功能。这些发现支持了新兴的概念,即CAR不仅是一种结构蛋白,而且还可能通过其与非受体蛋白激酶的结构相互作用介导在BTB上其他粘附蛋白(例如occludin)的磷酸化状态。内吞小泡介导的蛋白质运输。

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