人类和小鼠组织中视网膜下色素上皮细胞层沉积物的增强检测:成像锌作为年龄相关性黄斑变性的生物标志物(美国眼科学会论文)。

Transactions of the American Ophthalmological Society Pub Date : 2017-08-22 eCollection Date: 2017-08-01
Frederik J G M van Kuijk, Scott W McPherson, Heidi Roehrich
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摘要

目的:了解锌在年龄相关性黄斑变性(AMD)发病机制和预防中的明显矛盾作用,由于缺乏动物模型来检测视网膜下上皮沉积物(drusen),这是AMD的明确早期标志。使用Zinpyr-1进行的体外研究表明,drusen含有高水平的锌,但该探针不适合用于体内研究。本研究比较了Zinpyr-1和ZPP1(一种新的基于荧光素的锌探针),以评估ZPP1在家禽体内检测锌的潜力。方法:用荧光显微镜和共聚焦显微镜对探针制备的人亚rpe组织平片进行分析。我们分析了缺乏超氧化物歧化酶亚型1 (CuZn-SOD-KO)或亚型2 (Mn-SOD-RPE-KO)小鼠的亚rpe组织,并通过组织学证实了亚rpe沉积。结果:与zpyr -1相比,ZPP1对Drusen的检测数量和强度更高。使用ZPP1,在一名46岁无眼部病史的人类供体样本中检测到drusen,这表明ZPP1可能足够敏感,可以在早期检测到drusen。在CuZn-SOD KO小鼠中,ZPP1在10月龄时检测到亚rpe沉积,而Zinpyr-1则需要14月龄。结论:与zpyr -1相比,ZPP1对亚rpe沉积物的检测能力明显增强。这种增强的灵敏度将允许使用人类标本和小鼠模型对AMD中的锌进行更深入的分析。这可能导致一种灵敏的体内探针的发展,以加强锌在肾小球形成和AMD早期临床诊断中的作用的研究。
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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Enhanced Detection of Sub-Retinal Pigment Epithelial Cell Layer Deposits in Human and Murine Tissue: Imaging Zinc as a Biomarker for Age-Related Macular Degeneration (An American Ophthalmological Society Thesis).

Purpose: Understanding the apparent paradoxical role of zinc in the pathogenesis and prevention of age-related macular degeneration (AMD) has been limited by the lack of animal models for its detection in sub-retinal epithelial deposits (drusen), a definitive early hallmark of AMD. In-vitro studies using Zinpyr-1 showed drusen contained high levels of zinc, but the probe was not suitable for in-vivo studies. This study compares Zinpyr-1 to ZPP1, a new fluorescein-based probe for zinc, to assess the potential of ZPP1 for in-vivo detection of zinc in drusen.

Methods: Flat mounts of human sub-RPE tissue using the probes were analyzed by fluorescence and confocal microscopy. Flat mounts of sub-RPE tissue from mice deficient in superoxide dismutase isoform-1 (CuZn-SOD-KO) or isoform-2 (Mn-SOD-RPE-KO) were analyzed with sub-RPE deposits confirmed by histology.

Results: Drusen are detected in greater numbers and intensity with ZPP1 compared to Zinpyr-1. Using ZPP1, drusen was detected in a sample from a 46-year old human donor without ocular history, suggesting that ZPP1 might be sensitive enough to detect drusen at an early stage. With CuZn-SOD KO mice, ZPP1 detected sub-RPE deposits at 10 months of age, whereas Zinpyr-1 required 14 months.

Conclusion: Detection of sub-RPE deposits by ZPP1 was greatly enhanced compared to Zinpyr-1. This enhanced sensitivity will allow for more insightful analysis of zinc in AMD using human specimens and mouse models. This could result in the development of a sensitive in-vivo probe to enhance research on the role zinc in drusen formation and the early clinical diagnosis of AMD.

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