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Usher 综合征蛋白网络在视网膜中的功能及其与其他视网膜纤毛病的关系。

Usher syndrome protein network functions in the retina and their relation to other retinal ciliopathies.

机构信息

Institute of Zoology, Dept. Cell & Matrix Biology, Johannes Gutenberg University Mainz, Mainz, Germany,

出版信息

Adv Exp Med Biol. 2014;801:527-33. doi: 10.1007/978-1-4614-3209-8_67.

Abstract

The human Usher syndrome (USH) is the most frequent cause of combined hereditary deaf-blindness. USH is genetically and clinically heterogeneous: 15 chromosomal loci assigned to 3 clinical types, USH1-3. All USH1 and 2 proteins are organized into protein networks by the scaffold proteins harmonin (USH1C), whirlin (USH2D) and SANS (USH1G). This has contributed essentially to our current understanding of the USH protein function in the eye and the ear and explains why defects in proteins of different families cause very similar phenotypes. Ongoing in depth analyses of USH protein networks in the eye indicated cytoskeletal functions as well as roles in molecular transport processes and ciliary cargo delivery in photoreceptor cells. The analysis of USH protein networks revealed molecular links of USH to other ciliopathies, including non-syndromic inner ear defects and isolated retinal dystrophies but also to kidney diseases and syndromes like the Bardet-Biedl syndrome. These findings provide emerging evidence that USH is a ciliopathy molecularly related to other ciliopathies, which opens an avenue for common therapy strategies to treat these diseases.

摘要

人类先天性耳聋-色素性视网膜炎(Usher 综合征,USH)是遗传性聋盲中最常见的疾病。USH 是一种遗传异质性和临床异质性疾病,已发现 15 个基因座与 3 种临床类型(USH1、USH2 和 USH3)相关。所有的 USH1 和 USH2 蛋白均由连接蛋白 harmonin(USH1C)、whirlin(USH2D)和 SANS(USH1G)组装成蛋白网络。这对理解 USH 蛋白在眼和耳中的功能有重要贡献,也解释了为什么不同家族的蛋白缺陷会导致非常相似的表型。对眼内 USH 蛋白网络的深入分析表明,其具有细胞骨架功能,以及在光感受器细胞中的分子转运过程和纤毛货物运输中的作用。对 USH 蛋白网络的分析揭示了 USH 与其他纤毛病(包括非综合征性内耳缺陷和孤立性视网膜营养不良)、肾脏疾病以及 Bardet-Biedl 综合征等综合征之间的分子联系。这些发现为 USH 是一种与其他纤毛病相关的纤毛病提供了新的证据,为治疗这些疾病的共同治疗策略开辟了道路。

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