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논문 기본 정보

자료유형
학술저널
저자정보
Li Xiang (Sun Yat-Sen University) Peng Zhiming (Sun Yat-Sen University) Long Lingli (Sun Yat-Sen University) Lu Xiaofang (Sun Yat-Sen University) Zhu Kai (Sun Yat-Sen University) Tuo Ying (Sun Yat-Sen University) Chen Ningning (Sun Yat-Sen University) Zhao Xiaoyang (Sun Yat-Sen University) Wang Le (Sun Yat-Sen University) Wan Yong (Sun Yat-Sen University)
저널정보
대한생화학·분자생물학회 Experimental and Molecular Medicine Experimental and Molecular Medicine 제52권
발행연도
2020.12
수록면
1 - 14 (14page)
DOI
10.1038/s12276-020-00536-0

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Traditional therapeutic strategies for spinal cord injury (SCI) are insufficient to repair locomotor function because of the failure of axonal reconnection and neuronal regeneration in the injured central nervous system (CNS). Neural stem cell (NSC) transplantation has been considered a potential strategy and is generally feasible for repairing the neural circuit after SCI; however, the most formidable problem is that the neuronal differentiation rate of NSCs is quite limited. Therefore, it is essential to induce the neuronal differentiation of NSCs and improve the differentiation rate of NSCs in spinal cord repair. Our results demonstrate that both Wnt5a and miRNA200b-3p could promote NSC differentiation into neurons and that Wnt5a upregulated miRNA200b-3p expression through MAPK/JNK signaling to promote NSC differentiation into neurons. Wnt5a could reduce RhoA expression by upregulating miRNA200b-3p expression to inhibit activation of the RhoA/Rock signaling pathway, which has been reported to suppress neuronal differentiation. Overexpression of RhoA abolished the neurogenic capacity of Wnt5a and miRNA200b-3p. In vivo, miRNA200b-3p was critical for Wnt5a-induced NSC differentiation into neurons to promote motor functional and histological recovery after SCI by suppressing RhoA/Rock signaling. These findings provide more insight into SCI and help with the identification of novel treatment strategies.

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