학술논문
Deletion of IFT20 exclusively in the RPE ablates primary cilia and leads to retinal degeneration.
Document Type
Article
Author
Source
Subject
*RETINAL degeneration
*CILIA & ciliary motion
*PHOTORECEPTORS
*VISION disorders
*RHODOPSIN
*VISION
*HOMEOSTASIS
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Language
ISSN
1544-9173
Abstract
Vision impairment places a serious burden on the aging society, affecting the lives of millions of people. Many retinal diseases are of genetic origin, of which over 50% are due to mutations in cilia-associated genes. Most research on retinal degeneration has focused on the ciliated photoreceptor cells of the retina. However, the contribution of primary cilia in other ocular cell types has largely been ignored. The retinal pigment epithelium (RPE) is a monolayer epithelium at the back of the eye intricately associated with photoreceptors and essential for visual function. It is already known that primary cilia in the RPE are critical for its development and maturation; however, it remains unclear whether this affects RPE function and retinal tissue homeostasis. We generated a conditional knockout mouse model, in which IFT20 is exclusively deleted in the RPE, ablating primary cilia. This leads to defective RPE function, followed by photoreceptor degeneration and, ultimately, vision impairment. Transcriptomic analysis offers insights into mechanisms underlying pathogenic changes, which include transcripts related to epithelial homeostasis, the visual cycle, and phagocytosis. Due to the loss of cilia exclusively in the RPE, this mouse model enables us to tease out the functional role of RPE cilia and their contribution to retinal degeneration, providing a powerful tool for basic and translational research in syndromic and non-syndromic retinal degeneration. Non-ciliary mechanisms of IFT20 in the RPE may also contribute to pathogenesis and cannot be excluded, especially considering the increasing evidence of non-ciliary functions of ciliary proteins. Most research on retinal degeneration has focused on the ciliated photoreceptor cells, but the role of primary cilia in other ocular cell types has largely been ignored. This study shows that the primary cilium in the retinal pigment epithelium is essential for development and for the proper functioning of this tissue; its absence results in retinal degeneration. [ABSTRACT FROM AUTHOR]