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补体级联抑制在地图样萎缩中的研究进展。

Complement cascade inhibition in geographic atrophy: a review.

机构信息

Iveric Bio, 1249 South River Road, Suite 107, Cranbury, NJ, 08512, USA.

出版信息

Eye (Lond). 2022 Feb;36(2):294-302. doi: 10.1038/s41433-021-01765-x. Epub 2022 Jan 9.

Abstract

The pathophysiology of dry age-related macular degeneration (AMD) and specifically geographic atrophy (GA) has been linked to the complement cascade. This cascade is part of the innate immune system and is made up of the classical, alternative, and lectin pathways. The pathways comprise a system of plasma and membrane-associated serum proteins that are activated with identification of a nonself entity. A number of these proteins have been implicated in the development and progression of dry AMD. The three pathways converge at C3 and cascade down through C5, making both of these proteins viable targets for the treatment of dry AMD. In addition, there are a number of complement factors, CFB, CFD, CFH, and CFI, which are potential therapeutic targets as well. Several different complement-directed therapeutics are being studied for the treatment of dry AMD with the hope that one of these approaches will emerge as the first approved treatment for GA.

摘要

干性年龄相关性黄斑变性(AMD)的病理生理学,特别是地理萎缩(GA),与补体级联反应有关。该级联反应是先天免疫系统的一部分,由经典途径、替代途径和凝集素途径组成。这些途径包含一系列血浆和膜相关的血清蛋白,当识别出非自身实体时,这些蛋白被激活。许多这些蛋白质与干性 AMD 的发生和进展有关。三条途径在 C3 汇聚,并通过 C5 级联下降,使这两种蛋白质都成为干性 AMD 治疗的可行靶点。此外,还有许多补体因子,如 CFB、CFD、CFH 和 CFI,也是潜在的治疗靶点。目前正在研究几种不同的补体导向治疗方法来治疗干性 AMD,希望其中一种方法能成为 GA 的首个获批治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc1f/8807727/60385de9da04/41433_2021_1765_Fig1_HTML.jpg

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