| Literature DB >> 30224460 |
Feng Zhang1,2, Yaqing Wang1,2, Tao Wang1,2, Li Yao3, Sin Man Lam1, Xiahe Huang1, Junwan Fan1,2, Qin Wang1,2, Liang Liu1,2, Yisheng Jiang1,2, Hongsheng Zhang1, Lei Shi1, Mei Yu1, Guanghou Shui1, Yingchun Wang1, Fei Gao4, Xiaohui Zhang3, Zhiheng Xu5,2,6.
Abstract
Normal neural development is essential for the formation of neuronal networks and brain function. Cutaneous T cell lymphoma-associated antigen 5 (cTAGE5)/meningioma expressed antigen 6 (MEA6) plays a critical role in the secretion of proteins. However, its roles in the transport of nonsecretory cellular components and in brain development remain unknown. Here, we show that cTAGE5/MEA6 is important for brain development and function. Conditional knockout of cTAGE5/MEA6 in the brain leads to severe defects in neural development, including deficits in dendrite outgrowth and branching, spine formation and maintenance, astrocyte activation, and abnormal behaviors. We reveal that loss of cTAGE5/MEA6 affects the interaction between the coat protein complex II (COPII) components, SAR1 and SEC23, leading to persistent activation of SAR1 and defects in COPII vesicle formation and transport from the endoplasmic reticulum to the Golgi, as well as disturbed trafficking of membrane components in neurons. These defects affect not only the transport of materials required for the development of dendrites and spines but also the signaling pathways required for neuronal development. Because mutations in cTAGE5/MEA6 have been found in patients with Fahr's disease, our study potentially also provides insight into the pathogenesis of this disorder.Entities:
Keywords: COPII; MEA6; brain development; cTAGE5; vesicle trafficking
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Year: 2018 PMID: 30224460 PMCID: PMC6176567 DOI: 10.1073/pnas.1804083115
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205