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眼部内稳态和疾病中的窖腔和非窖腔窖蛋白-1。

Caveolar and non-Caveolar Caveolin-1 in ocular homeostasis and disease.

机构信息

Department of Physiology, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA; Department of Ophthalmology, Dean A. McGee Eye Institute, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA.

Department of Ophthalmology, Duke Eye Center, Duke University, Durham, NC, USA.

出版信息

Prog Retin Eye Res. 2022 Nov;91:101094. doi: 10.1016/j.preteyeres.2022.101094. Epub 2022 Jun 18.

Abstract

Caveolae, specialized plasma membrane invaginations present in most cell types, play important roles in multiple cellular processes including cell signaling, lipid uptake and metabolism, endocytosis and mechanotransduction. They are found in almost all cell types but most abundant in endothelial cells, adipocytes and fibroblasts. Caveolin-1 (Cav1), the signature structural protein of caveolae was the first protein associated with caveolae, and in association with Cavin1/PTRF is required for caveolae formation. Genetic ablation of either Cav1 or Cavin1/PTRF downregulates expression of the other resulting in loss of caveolae. Studies using Cav1-deficient mouse models have implicated caveolae with human diseases such as cardiomyopathies, lipodystrophies, diabetes and muscular dystrophies. While caveolins and caveolae are extensively studied in extra-ocular settings, their contributions to ocular function and disease pathogenesis are just beginning to be appreciated. Several putative caveolin/caveolae functions are relevant to the eye and Cav1 is highly expressed in retinal vascular and choroidal endothelium, Müller glia, the retinal pigment epithelium (RPE), and the Schlemm's canal endothelium and trabecular meshwork cells. Variants at the CAV1/2 gene locus are associated with risk of primary open angle glaucoma and the high risk HTRA1 variant for age-related macular degeneration is thought to exert its effect through regulation of Cav1 expression. Caveolins also play important roles in modulating retinal neuroinflammation and blood retinal barrier permeability. In this article, we describe the current state of caveolin/caveolae research in the context of ocular function and pathophysiology. Finally, we discuss new evidence showing that retinal Cav1 exists and functions outside caveolae.

摘要

小窝,存在于大多数细胞类型中的特殊质膜内陷,在包括细胞信号转导、脂质摄取和代谢、内吞作用和机械转导在内的多种细胞过程中发挥重要作用。它们存在于几乎所有的细胞类型中,但在血管内皮细胞、脂肪细胞和成纤维细胞中最为丰富。小窝蛋白-1(Cav1),小窝的标志性结构蛋白,是第一个与小窝相关的蛋白质,与Cavin1/PTRF 结合是小窝形成所必需的。Cav1 或 Cavin1/PTRF 的基因缺失会下调另一种蛋白的表达,导致小窝缺失。使用 Cav1 缺陷型小鼠模型的研究表明,小窝与人类疾病有关,如心肌病、脂肪营养不良、糖尿病和肌肉营养不良。虽然小窝蛋白和小窝在眼外环境中得到了广泛研究,但它们对眼部功能和疾病发病机制的贡献才刚刚开始被认识。几个假定的小窝蛋白/小窝功能与眼睛有关,Cav1 在视网膜血管和脉络膜内皮细胞、Müller 胶质细胞、视网膜色素上皮(RPE)和施莱姆氏管内皮细胞和小梁网细胞中高度表达。CAV1/2 基因座的变异与原发性开角型青光眼的风险相关,而与年龄相关性黄斑变性相关的高风险 HTRA1 变异体被认为通过调节 Cav1 表达来发挥作用。小窝蛋白还在调节视网膜神经炎症和血视网膜屏障通透性方面发挥着重要作用。在本文中,我们将描述小窝蛋白/小窝在眼部功能和病理生理学方面的研究现状。最后,我们讨论了新的证据表明,视网膜 Cav1 存在于小窝之外并发挥作用。

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