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PCP 蛋白反向蛋白调节睾丸功能通过细胞骨架组织的变化肌动蛋白和微管。

PCP Protein Inversin Regulates Testis Function Through Changes in Cytoskeletal Organization of Actin and Microtubules.

机构信息

The Second Affiliated Hospital and Yuying Children's Hospital, Wenzhou Medical University, Wenzhou, Zhejiang 325027, China.

Institute of Reproductive Medicine, Nantong University School of Medicine, Nantong, Jiangsu 226001, China.

出版信息

Endocrinology. 2022 Apr 1;163(4). doi: 10.1210/endocr/bqac009.

Abstract

Inversin is an integrated component of the Frizzled (Fzd)/Dishevelled (Dvl)/Diversin planar cell polarity (PCP) complex that is known to work in concert with the Van Gogh-like protein (eg, Vangl2)/Prickle PCP complex to support tissue and organ development including the brain, kidney, pancreas, and others. These PCP protein complexes are also recently shown to confer developing haploid spermatid PCP to support spermatogenesis in adult rat testes. However, with the exception of Dvl3 and Vangl2, other PCP proteins have not been investigated in the testis. Herein, we used the technique of RNA interference (RNAi) to examine the role of inversin (Invs) in Sertoli cell (SC) and testis function by corresponding studies in vitro and in vivo. When inversin was silenced by RNAi using specific small interfering RNA duplexes by transfecting primary cultures of SCs in vitro or testes in vivo, it was shown that inversin knockdown (KD) perturbed the SC tight junction-barrier function in vitro and in vivo using corresponding physiological and integrity assays. More important, inversin exerted its regulatory effects through changes in the organization of the actin and microtubule cytoskeletons, including reducing the ability of their polymerization. These changes, in turn, induced defects in spermatogenesis by loss of spermatid polarity, disruptive distribution of blood-testis barrier-associated proteins at the SC-cell interface, appearance of multinucleated round spermatids, and defects in the release of sperm at spermiation.

摘要

内反转蛋白是卷曲(Fzd)/离散(Dvl)/ Diversin 平面细胞极性(PCP)复合物的一个组成部分,已知该复合物与梵高样蛋白(例如,Vangl2)/ Prickle PCP 复合物协同作用,以支持组织和器官发育,包括大脑、肾脏、胰腺等。这些 PCP 蛋白复合物最近也被证明赋予了正在发育的单倍体精原细胞 PCP,以支持成年大鼠睾丸中的精子发生。然而,除了 Dvl3 和 Vangl2 之外,其他 PCP 蛋白在睾丸中尚未得到研究。在此,我们使用 RNA 干扰(RNAi)技术通过体外和体内相应的研究来检查内反转蛋白(Invs)在支持细胞(SCs)和睾丸功能中的作用。当通过转染体外 SC 原代培养物或体内睾丸的特异性小干扰 RNA 双链体沉默内反转蛋白时,证明内反转蛋白敲低(KD)通过相应的生理和完整性测定体外和体内干扰了 SC 紧密连接-屏障功能。更重要的是,内反转蛋白通过改变肌动蛋白和微管细胞骨架的组织发挥其调节作用,包括降低其聚合能力。这些变化反过来通过丧失精子极性、血睾屏障相关蛋白在 SC 细胞界面的分布紊乱、多倍体圆形精子的出现以及精子排放时的缺陷,导致精子发生缺陷。

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