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杂合 CRX 突变猫(CRX)中的代谢变化和视网膜重塑。

Metabolic changes and retinal remodeling in Heterozygous CRX mutant cats (CRX).

机构信息

Small Animal Clinical Sciences, Michigan State University, 736 Wilson Road, East Lansing, MI, USA.

Ophthalmology, Moran Eye Center, University of Utah, Salt Lake City, UT, USA.

出版信息

Exp Eye Res. 2023 Oct;235:109630. doi: 10.1016/j.exer.2023.109630. Epub 2023 Aug 23.

Abstract

CRX is a transcription factor essential for normal photoreceptor development and survival. The CRX cat has a naturally occurring truncating mutation in CRX and is a large animal model for dominant Leber congenital amaurosis. This study investigated retinal remodeling that occurs as photoreceptors degenerate. CRX cats from 6 weeks to 10 years of age were investigated. In vivo structural changes of retinas were analyzed by fundus examination, confocal scanning laser ophthalmoscopy and spectral domain optical coherence tomography. Histologic analyses included immunohistochemistry for computational molecular phenotyping with macromolecules and small molecules. Affected cats had a cone-led photoreceptor degeneration starting in the area centralis. Initially there was preservation of inner retinal cells such as bipolar, amacrine and horizontal cells but with time migration of the deafferented neurons occurred. Early in the process of degeneration glial activation occurs ultimately resulting in formation of a glial seal. With progression the macula-equivalent area centralis developed severe atrophy including loss of retinal pigmentary epithelium. Microneuroma formation occured in advanced stages as more marked retinal remodeling occurred. This study indicates that retinal degeneration in the Crx cat retina follows the progressive, phased revision of retina that have been previously described for retinal remodeling. These findings suggest that therapy dependent on targeting inner retinal cells may be useful in young adults with preserved inner retinas prior to advanced stages of retinal remodeling and neuronal cell loss.

摘要

CRX 是一种对正常感光细胞发育和存活至关重要的转录因子。CRX 猫的 CRX 中存在自然发生的截断突变,是一种用于研究显性先天性黑蒙 Leber 的大型动物模型。本研究调查了感光细胞变性时发生的视网膜重塑。研究了 6 周至 10 岁的 CRX 猫。通过眼底检查、共焦扫描激光检眼镜和谱域光学相干断层扫描分析视网膜的体内结构变化。组织学分析包括用大分子和小分子进行计算分子表型的免疫组织化学。受影响的猫的中央凹区有以视锥细胞为主的感光细胞变性。最初,双极细胞、无长突细胞和水平细胞等内视网膜细胞得以保留,但随着时间的推移,去传入神经元发生迁移。在变性过程的早期,神经胶质细胞激活,最终导致神经胶质封闭。随着病情的进展,黄斑等效中央凹区发生严重萎缩,包括视网膜色素上皮丧失。在更明显的视网膜重塑发生的晚期,形成微神经瘤。本研究表明,Crx 猫视网膜的退行性变遵循先前描述的视网膜重塑的渐进、分阶段修订。这些发现表明,在视网膜重塑和神经元细胞丢失的晚期之前,针对内视网膜细胞的靶向治疗可能对保留内视网膜的年轻成年人有用。

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