| Literature DB >> 32868309 |
Tomomi Okajima1, Yichen Gu1, Rin-Ichiro Teruya2, Sarasa Yano1, Takumi Taketomi2, Ban Sato3, Tomoki Chiba3,4, Fuminori Tsuruta5,4,6.
Abstract
Microglia are resident macrophages that are critical for brain development and homeostasis. Microglial morphology is dynamically changed during postnatal stages, leading to regulating synaptogenesis and synapse pruning. Moreover, it has been well known that the shape of microglia is also altered in response to the detritus of the apoptotic cells and pathogens such as bacteria and viruses. Although the morphologic changes are crucial for acquiring microglial functions, the exact mechanism which controls their morphology is not fully understood. Here, we report that the FAT atypical cadherin family protein, FAT3, regulates the morphology of microglial cell line, BV2. We found that the shape of BV2 becomes elongated in a high-nutrient medium. Using microarray analysis, we identified that FAT3 expression is induced by culturing with a high-nutrient medium. In addition, we found that purinergic analog, hypoxanthine, promotes FAT3 expression in BV2 and mouse primary microglia. FAT3 expression induced by hypoxanthine extends the time of sustaining the elongated forms in BV2. These data suggest that the hypoxanthine-FAT3 axis is a novel pathway associated with microglial morphology. Our data provide a possibility that FAT3 may control microglial transitions involved in their morphologic changes during the postnatal stages in vivo.Entities:
Keywords: FAT3; HPRT1; Lesch–Nyhan syndrome; hypoxanthine; microglia; morphogenesis
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Year: 2020 PMID: 32868309 PMCID: PMC7768282 DOI: 10.1523/ENEURO.0056-20.2020
Source DB: PubMed Journal: eNeuro ISSN: 2373-2822