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CD73 控制眼内腺苷水平,保护视网膜免受光诱导的光毒性。

CD73 controls ocular adenosine levels and protects retina from light-induced phototoxicity.

机构信息

MediCity Research Laboratory and InFLAMES Flagship, University of Turku, Tykistökatu 6A, 20520, Turku, Finland.

Experimentica UAB, Vilnius, Lithuania.

出版信息

Cell Mol Life Sci. 2022 Feb 25;79(3):152. doi: 10.1007/s00018-022-04187-4.

DOI:10.1007/s00018-022-04187-4
PMID:35212809
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8881442/
Abstract

ATP and adenosine have emerged as important signaling molecules involved in vascular remodeling, retinal functioning and neurovascular coupling in the mammalian eye. However, little is known about the regulatory mechanisms of purinergic signaling in the eye. Here, we used three-dimensional multiplexed imaging, in situ enzyme histochemistry, flow cytometric analysis, and single cell transcriptomics to characterize the whole pattern of purine metabolism in mouse and human eyes. This study identified ecto-nucleoside triphosphate diphosphohydrolase-1 (NTPDase1/CD39), NTPDase2, and ecto-5'-nucleotidase/CD73 as major ocular ecto-nucleotidases, which are selectively expressed in the photoreceptor layer (CD73), optic nerve head, retinal vasculature and microglia (CD39), as well as in neuronal processes and cornea (CD39, NTPDase2). Specifically, microglial cells can create a spatially arranged network in the retinal parenchyma by extending and retracting their branched CD39/CD73 processes and forming local "purinergic junctions" with CD39/CD73 neuronal cell bodies and CD39/CD73 retinal blood vessels. The relevance of the CD73-adenosine pathway was confirmed by flash electroretinography showing that pharmacological inhibition of adenosine production by injection of highly selective CD73 inhibitor PSB-12489 in the vitreous cavity of dark-adapted mouse eyes rendered the animals hypersensitive to prolonged bright light, manifested as decreased a-wave and b-wave amplitudes. The impaired electrical responses of retinal cells in PSB-12489-treated mice were not accompanied by decrease in total thickness of the retina or death of photoreceptors and retinal ganglion cells. Our study thus defines ocular adenosine metabolism as a complex and spatially integrated network and further characterizes the critical role of CD73 in maintaining the functional activity of retinal cells.

摘要

三磷酸腺苷和腺苷已成为哺乳动物眼睛中参与血管重塑、视网膜功能和神经血管耦合的重要信号分子。然而,关于眼睛中嘌呤能信号的调节机制知之甚少。在这里,我们使用三维多重成像、原位酶组织化学、流式细胞分析和单细胞转录组学来描述小鼠和人眼中嘌呤代谢的整个模式。这项研究确定了外核苷酸三磷酸二磷酸水解酶-1 (NTPDase1/CD39)、NTPDase2 和外 5'-核苷酸酶/CD73 为主要的眼外核苷酸酶,它们选择性地表达在光感受器层 (CD73)、视神经头部、视网膜血管和小胶质细胞 (CD39) 中,以及在神经元过程和角膜 (CD39、NTPDase2) 中。具体来说,小胶质细胞可以通过伸展和缩回其分支 CD39/CD73 过程,在视网膜实质中创建一个空间排列的网络,并与 CD39/CD73 神经元细胞体和 CD39/CD73 视网膜血管形成局部“嘌呤能连接”。通过闪光视网膜电图证实了 CD73-腺苷途径的相关性,向暗适应小鼠眼睛的玻璃体腔注射高度选择性的 CD73 抑制剂 PSB-12489 抑制腺苷产生,导致动物对长时间强光敏感,表现为 a 波和 b 波幅度降低。PSB-12489 处理的小鼠视网膜细胞的电反应受损,并不伴有视网膜总厚度的减少或光感受器和视网膜神经节细胞的死亡。因此,我们的研究将眼部腺苷代谢定义为一个复杂的、空间整合的网络,并进一步描述了 CD73 在维持视网膜细胞功能活性方面的关键作用。

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Biological insights from the direct measurement of purine release.嘌呤释放的直接测量带来的生物学启示。
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