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Cited 17 time in webofscience Cited 16 time in scopus
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Sequential phosphorylation of NDEL1 by the DYRK2-GSK3 beta complex is critical for neuronal morphogenesis

Authors
Woo, YoungsikKim, Soo JeongSuh, Bo KyoungKwak, YongdoJung, Hyun-JinTruong Thi My NhungDong Jin MunHong, Ji-HoNoh, Su-JinKim, SeunghyunLee, AhryoungBaek, Seung TaeMinh Dang NguyenChoe, YoungshikPark, Sang Ki
Issue Date
Dec-2019
Publisher
ELIFE SCIENCES PUBLICATIONS LTD
Citation
ELIFE, v.8
Journal Title
ELIFE
Volume
8
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/657
DOI
10.7554/eLife.50850
ISSN
2050-084X
Abstract
Neuronal morphogenesis requires multiple regulatory pathways to appropriately determine axonal and dendritic structures, thereby to enable the functional neural connectivity. Yet, however, the precise mechanisms and components that regulate neuronal morphogenesis are still largely unknown. Here, we newly identified the sequential phosphorylation of NDEL1 critical for neuronal morphogenesis through the human kinome screening and phospho-proteomics analysis of NDEL1 from mouse brain lysate. DYRK2 phosphorylates NDEL1 S336 to prime the phosphorylation of NDEL1 S332 by GSK3 beta. TARA, an interaction partner of NDEL1, scaffolds DYRK2 and GSK3 beta to form a tripartite complex and enhances NDEL1 S336/S332 phosphorylation. This dual phosphorylation increases the filamentous actin dynamics. Ultimately, the phosphorylation enhances both axonal and dendritic outgrowth and promotes their arborization. Together, our findings suggest the NDEL1 phosphorylation at S336/S332 by the TARA-DYRK2-GSK3 beta complex as a novel regulatory mechanism underlying neuronal morphogenesis.
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연구본부 (뇌발달질환 연구그룹)
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