Lack of retinal degeneration in a Dram2 knockout mouse model

IF 1.5 4区 心理学 Q4 NEUROSCIENCES
Kuanxiang Sun , Junyao Chen , Yudi Fan , Jinrui Cai , Xiaoyan Jiang , Wenjing Liu , Xianjun Zhu
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Abstract

Damage-regulated autophagy modulator 2 (DRAM2) is a homologue of the DRAM family protein, which can induce autophagy process. In the retina, DRAM2 is located to the inner segment of photoreceptors, the apical surface of retinal pigment epithelial (RPE) cells, and the lysosome. Pathogenic variants of DRAM2 lead to autosomal recessive Cone-rod dystrophy 21 (CORD21). Cone-rod dystrophy is characterised by primary cone involvement, or sometimes simultaneous cone and rod loss, thus leading to decreased visual acuity, colour vision deficits, photophobia, and decreased sensitivity of the central visual field. However, the mechanisms underlying DRAM2 related retinal diseases remained unclear. To further explore the role of Dram2 in the retina, we generated Dram2 knockout mice (KO) by CRISPR/Cas-9 technology and demonstrated that expression of DRAM2 was abolished in KO retinas. Dram2 ablation failed to manifest any retinal degenerative phenotypes. Dram2 KO did not exhibit visible defect in photo response and the overt structure of the retinas. Immunostaing analysis using antibodies against cone opsins revealed no detectable loss of cone cells. Moreover, no visible change was observed in the expression and localisation of rhodopsin and other membrane disc proteins in Dram2 KO retinas and no gliosis and apoptosis were detected in KO mice. In summary, these data revealed lack of overt retinal degeneration in Dram2 KO model and emphasized the importance of further investigation of the mechanisms underlying Cone-rod dystrophy 21.
Dram2 基因敲除小鼠模型缺乏视网膜变性。
损伤调控自噬调节因子2(DRAM2)是DRAM家族蛋白的同源物,可诱导自噬过程。在视网膜中,DRAM2 位于感光器内节、视网膜色素上皮细胞(RPE)顶端表面和溶酶体。DRAM2 的致病变体会导致常染色体隐性遗传的圆锥杆状营养不良症 21(CORD21)。锥状杆营养不良症的特点是原发性锥状体受累,有时锥状体和杆状体同时丧失,从而导致视力下降、色觉障碍、畏光和中央视野敏感度降低。然而,DRAM2 相关视网膜疾病的发病机制仍不清楚。为了进一步探索Dram2在视网膜中的作用,我们通过CRISPR/Cas-9技术产生了Dram2基因敲除小鼠(KO),并证明DRAM2在KO视网膜中的表达被取消。Dram2 消减未能表现出任何视网膜变性表型。Dram2 KO没有表现出明显的光反应缺陷和视网膜的明显结构缺陷。使用针对视锥蛋白的抗体进行的免疫测定分析表明,没有发现视锥细胞的损失。此外,Dram2 KO 小鼠视网膜中的视紫红质和其他膜盘蛋白的表达和定位没有发生明显变化,也没有检测到神经胶质增生和细胞凋亡。总之,这些数据揭示了 Dram2 KO 模型缺乏明显的视网膜变性,并强调了进一步研究 21 型锥体-杆状营养不良症的机制的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Vision Research
Vision Research 医学-神经科学
CiteScore
3.70
自引率
16.70%
发文量
111
审稿时长
66 days
期刊介绍: Vision Research is a journal devoted to the functional aspects of human, vertebrate and invertebrate vision and publishes experimental and observational studies, reviews, and theoretical and computational analyses. Vision Research also publishes clinical studies relevant to normal visual function and basic research relevant to visual dysfunction or its clinical investigation. Functional aspects of vision is interpreted broadly, ranging from molecular and cellular function to perception and behavior. Detailed descriptions are encouraged but enough introductory background should be included for non-specialists. Theoretical and computational papers should give a sense of order to the facts or point to new verifiable observations. Papers dealing with questions in the history of vision science should stress the development of ideas in the field.
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