黄斑变性眼游离视蛋白的生化测定:探讨延迟暗适应的11-CIS视网膜缺陷假说(美国眼科学会论文)。

Transactions of the American Ophthalmological Society Pub Date : 2017-08-22 eCollection Date: 2017-08-01
Anne Hanneken, Thomas Neikirk, Jennifer Johnson, Masahiro Kono
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引用次数: 0

摘要

目的:验证黄斑变性患者延迟暗适应是由于游离无配体视蛋白(载脂蛋白视蛋白)过量和视杆外节11-顺式视网膜视色团缺乏的假设。方法:在2-24小时内,从有黄斑变性和无黄斑变性的供体中采集50只尸体解剖眼。后期。制定了允许正常人眼在死亡和去核后适应黑暗的方案。优化了纯化棒外段的生化方法,并用紫外可见扫描光谱法测定了视紫红质和载视蛋白的浓度。通过测定加入11-顺式视网膜前后视紫红质吸收光谱的差异来计算载视蛋白的存在。结果:正常眼20只,供体眼16只,均为黄斑变性早期、中期和晚期。通过在弱光下采集整个球体,将其转移到黑暗(防光)罐中,并使用红外光和图像转换器对球体进行解剖,以实现对黑暗的适应。添加11-顺式视网膜后,在阳性对照中很容易检测到载脂蛋白。正常尸检的眼睛没有发现载脂蛋白的证据。黄斑变性的眼睛也没有显示载脂蛋白的证据,无论疾病的严重程度。结论:已经建立了研究人体解剖眼暗适应的方法。与年龄相关的黄斑变性的眼睛不显示缺乏11-顺式视网膜或过量载脂蛋白视蛋白在杆外段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Biochemical Measurements of Free Opsin in Macular Degeneration Eyes: Examining the 11-<i>CIS</i> Retinal Deficiency Hypothesis of Delayed Dark Adaptation (An American Ophthalmological Society Thesis).

Biochemical Measurements of Free Opsin in Macular Degeneration Eyes: Examining the 11-<i>CIS</i> Retinal Deficiency Hypothesis of Delayed Dark Adaptation (An American Ophthalmological Society Thesis).

Biochemical Measurements of Free Opsin in Macular Degeneration Eyes: Examining the 11-<i>CIS</i> Retinal Deficiency Hypothesis of Delayed Dark Adaptation (An American Ophthalmological Society Thesis).

Biochemical Measurements of Free Opsin in Macular Degeneration Eyes: Examining the 11-CIS Retinal Deficiency Hypothesis of Delayed Dark Adaptation (An American Ophthalmological Society Thesis).

Purpose: To test the hypothesis that delayed dark adaptation in patients with macular degeneration is due to an excess of free unliganded opsin (apo-opsin) and a deficiency of the visual chromophore, 11-cis retinal, in rod outer segments.

Methods: A total of 50 human autopsy eyes were harvested from donors with and without macular degeneration within 2-24 hrs. postmortem. Protocols were developed which permitted dark adaptation of normal human eyes after death and enucleation. Biochemical methods of purifying rod outer segments were optimized and the concentration of rhodopsin and apo-opsin was measured with UV-visible scanning spectroscopy. The presence of apo-opsin was calculated by measuring the difference in the rhodopsin absorption spectra before and after the addition of 11-cis retinal.

Results: A total of 20 normal eyes and 16 eyes from donors with early, intermediate and advanced stages of macular degeneration were included in the final analysis. Dark adaptation was achieved by harvesting whole globes in low light, transferring into dark (light-proof) canisters and dissecting the globes using infrared light and image converters for visualization. Apo-opsin was readily detected in positive controls after the addition of 11-cis retinal. Normal autopsy eyes showed no evidence of apo-opsin. Eyes with macular degeneration also showed no evidence of apo-opsin, regardless of the severity of disease.

Conclusions: Methods have been developed to study dark adaptation in human autopsy eyes. Eyes with age-related macular degeneration do not show a deficiency of 11-cis retinal or an excess of apo-opsin within rod outer segments.

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