| Literature DB >> 35510502 |
Shuwei Xie1, Carter Dierlam2, Ellie Smith2, Ramon Duran2, Allana Williams2, Angelina Davis3, Danita Mathew2, Naava Naslavsky1, Jyoti Iyer2, Steve Caplan1,4.
Abstract
The mammalian retromer consists of subunits VPS26 (either VPS26A or VPS26B), VPS29 and VPS35, and a loosely associated sorting nexin (SNX) heterodimer or a variety of other SNX proteins. Despite involvement in yeast and mammalian cell trafficking, the role of retromer in development is poorly understood, and its impact on primary ciliogenesis remains unknown. Using CRISPR/Cas9 editing, we demonstrate that vps-26-knockout worms have reduced brood sizes, impaired vulval development and decreased body length, all of which have been linked to ciliogenesis defects. Although preliminary studies did not identify worm ciliary defects, and impaired development limited additional ciliogenesis studies, we turned to mammalian cells to investigate the role of retromer in ciliogenesis. VPS35 localized to the primary cilium of mammalian cells, and depletion of VPS26, VPS35, VPS29, SNX1, SNX2, SNX5 or SNX27 led to decreased ciliogenesis. Retromer also coimmunoprecipitated with the centriolar protein, CP110 (also known as CCP110), and was required for its removal from the mother centriole. Herein, we characterize new roles for retromer in C. elegans development and in the regulation of ciliogenesis in mammalian cells, suggesting a novel role for retromer in CP110 removal from the mother centriole.Entities:
Keywords: CP110; Centrosome; Ciliogenesis; Retromer; SNX1; SNX2; SNX27; SNX5; VPS26; VPS29; VPS35
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Year: 2022 PMID: 35510502 PMCID: PMC9189432 DOI: 10.1242/jcs.259396
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.235