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通过人视杆视蛋白的异位表达恢复视力

Restoration of Vision with Ectopic Expression of Human Rod Opsin.

作者信息

Cehajic-Kapetanovic Jasmina, Eleftheriou Cyril, Allen Annette E, Milosavljevic Nina, Pienaar Abigail, Bedford Robert, Davis Katherine E, Bishop Paul N, Lucas Robert J

机构信息

Centre for Ophthalmology and Vision Sciences, Institute of Human Development, University of Manchester, Manchester M13 9PT, UK; Manchester Royal Eye Hospital, CMFT, Manchester Academic Health Sciences Centre, Manchester M13 9NT, UK.

Faculty of Life Sciences, University of Manchester, Oxford Road, Manchester M13 9PT, UK.

出版信息

Curr Biol. 2015 Aug 17;25(16):2111-22. doi: 10.1016/j.cub.2015.07.029. Epub 2015 Jul 30.

Abstract

Many retinal dystrophies result in photoreceptor loss, but the inner retinal neurons can survive, making them potentially amenable to emerging optogenetic therapies. Here, we show that ectopically expressed human rod opsin, driven by either a non-selective or ON-bipolar cell-specific promoter, can function outside native photoreceptors and restore visual function in a mouse model of advanced retinal degeneration. Electrophysiological recordings from retinal explants and the visual thalamus revealed changes in firing (increases and decreases) induced by simple light pulses, luminance increases, and naturalistic movies in treated mice. These responses could be elicited at light intensities within the physiological range and substantially below those required by other optogenetic strategies. Mice with rod opsin expression driven by the ON-bipolar specific promoter displayed behavioral responses to increases in luminance, flicker, coarse spatial patterns, and elements of a natural movie at levels of contrast and illuminance (≈50-100 lux) typical of natural indoor environments. These data reveal that virally mediated ectopic expression of human rod opsin can restore vision under natural viewing conditions and at moderate light intensities. Given the inherent advantages in employing a human protein, the simplicity of this intervention, and the quality of vision restored, we suggest that rod opsin merits consideration as an optogenetic actuator for treating patients with advanced retinal degeneration.

摘要

许多视网膜营养不良会导致光感受器丧失,但视网膜内层神经元能够存活,这使得它们有可能适用于新兴的光遗传学疗法。在这里,我们表明,由非选择性或视锥双极细胞特异性启动子驱动的异位表达的人视杆视蛋白,能够在天然光感受器之外发挥作用,并在晚期视网膜变性的小鼠模型中恢复视觉功能。来自视网膜外植体和视觉丘脑的电生理记录显示,在经治疗的小鼠中,简单光脉冲、亮度增加和自然电影诱导了放电变化(增加和减少)。这些反应可以在生理范围内的光强度下引发,并且大大低于其他光遗传学策略所需的光强度。由视锥双极特异性启动子驱动视杆视蛋白表达的小鼠,在自然室内环境典型的对比度和照度(约50 - 100勒克斯)水平下,对亮度增加、闪烁、粗糙空间模式和自然电影元素表现出行为反应。这些数据表明,病毒介导的人视杆视蛋白异位表达能够在自然观察条件和中等光强度下恢复视力。鉴于使用人类蛋白质的固有优势、这种干预的简单性以及恢复的视力质量,我们建议视杆视蛋白值得作为一种光遗传学激活剂来考虑,用于治疗晚期视网膜变性患者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4681/4540256/6ebd5e6bb7a9/gr1.jpg

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