Wnt/PCP pathway regulates the migration and neural differentiation of mesenchymal stem cells in vitro

间充质干细胞 WNT3A型 罗亚 神经干细胞 Wnt信号通路 细胞生物学 归巢(生物学) 内斯汀 化学 干细胞 生物 信号转导 生态学
作者
Panpan Yao,Qin Yu,Lujie Zhu,Jingxian Li,Xueyuan Zhou,Lili Wu,Yongyi Cai,Hongmei Shen,Liping Zhou
出处
期刊:Folia Histochemica Et Cytobiologica [VM Media Sp zo.o. - VMGroup SK]
卷期号:60 (1): 44-54 被引量:3
标识
DOI:10.5603/fhc.a2022.0006
摘要

Mesenchymal stem cells (MSCs) are an excellent donor graft source due to their potential for self-renewal and multidirectional differentiation. However, the potential mechanisms involved in MSC homing and neural differentiation are still unclear. The purpose of this study was to explore the effects of a chemokine, SDF-1a, and Wnt3a ligand on rat MSCs' migration and b-mercaptoethanol (BME)-induced neural differentiation of MSCs.MSCs were isolated from rat bone marrow and cultured in vitro to passage 3. Scratch tests and transwell assays were used to estimate the effects of SDF-1a (25 ng/mL) and Wnt3a (10 ng/mL) on the migration of MSCs. The expression of Wnt/PCP pathway proteins RhoA, c-Jun, ATF2, and Wnt3a were assessed by Western blot. The 5 mM BME-induced neural differentiation of MSCs was determined by immunofluorescence to detect neuron- and astrocyte-specific markers such as nestin, GFAP, and Olig2.Wnt3a promoted the migration ability of MSCs and regulated the expression of RhoA, c-Jun, and ATF2 proteins. MSCs could differentiate into neural stem cells and astrocytes. Wnt3a enhanced BME induced neurogenesis in MSCs by increasing the protein expression of RhoA, c-Jun, and Wnt3a.The present study demonstrated that the Wnt/PCP pathway promotes migration and neural differentiation of rat MSC.
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