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Differential requirements for retinal degeneration slow intermolecular disulfide-linked oligomerization in rods versus cones

机译:视杆和视锥中视网膜变性的慢速分子间二硫键相关低聚反应的差异性要求

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摘要

It is commonly assumed that the ultrastructural organization of the rim region of outer segment (OS) discs in rods and lamellae in cones requires functional retinal degeneration slow/rod outer segment membrane protein 1 (Rds/Rom-1) complexes. Cysteine-150 (C150) in Rds has been implicated in intermolecular disulfide bonding essential for functional Rds complexes. Transgenic mice containing the Rds C150S mutation (C150S-Rds) failed to form higher-order Rds oligomers, although interactions between C150S-Rds and Rom-1 occurred in rods, but not in cones. C150S-Rds mice exhibited marked early-onset reductions in cone function and abnormal OS structure. In contrast, C150S-Rds expression in rods partly rescued the rds+/− phenotype. Although C150S-Rds was detected in the OSs in rods and cones, a substantial percentage of C150S-Rds and cone opsins were mislocalized to different cellular compartments in cones. The results of this study provide novel insights into the importance of C150 in Rds oligomerization and the differences in Rds requirements in rods versus cones. The apparent OS structural differences between rods and cones may cause cones to be more susceptible to the elimination of higher-order Rds/Rom-1 oligomers (e.g. as mediated by mutation of the Rds C150 residue).
机译:通常认为,杆中外段(OS)盘的边缘和视锥细胞中的薄片的超微结构需要功能性视网膜变性慢/杆外段膜蛋白1(Rds / Rom-1)复合物。 Rds中的半胱氨酸150(C150)与功能性Rds络合物必不可少的分子间二硫键有关。尽管C150S-Rds和Rom-1之间的相互作用发生在杆中,而不是在视锥细胞中发生,但是包含Rds C150S突变的转基因小鼠(C150S-Rds)未能形成更高阶的Rds低聚物。 C150S-Rds小鼠在锥体功能和异常OS结构方面表现出明显的早期发作减少。相反,杆中的C150S-Rds表达部分挽救了rds +/-表型。尽管在杆和视锥细胞的OS中检测到C150S-Rds,但相当大比例的C150S-Rds和视锥蛋白视锥细胞定位不正确。这项研究的结果提供了对C150在Rds低聚中的重要性以及棒与锥中Rds要求差异的新颖见解。视锥细胞和视锥细胞之间明显的OS结构差异可能导致视锥细胞更易于消除高阶Rds / Rom-1低聚物(例如,由Rds C150残基的突变介导)。

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