miR-124-3p regulates the proliferation and differentiation of retinal progenitor cells through SEPT10

被引:0
|
作者
Bingqiao Shen
Huiqin Gao
Dandan Zhang
Huan Yu
Junjue Chen
Shouyue Huang
Ping Gu
Yisheng Zhong
机构
[1] Ruijin Hospital,Department of Ophthalmology
[2] Shanghai Jiaotong University School of Medicine,Department of Ophthalmology, Ninth People’s Hospital Affiliated Medical School
[3] Shanghai Jiaotong University,undefined
来源
Cell and Tissue Research | 2023年 / 392卷
关键词
Retinal progenitor cells; MicroRNA; Proliferation; Differentiation;
D O I
暂无
中图分类号
学科分类号
摘要
Retinal degenerative diseases such as glaucoma, retinitis pigmentosa, and age-related macular degeneration pose serious threats to human visual health due to lack of effective therapeutic approaches. In recent years, the transplantation of retinal progenitor cells (RPCs) has shown increasing promise in the treatment of these diseases; however, the application of RPC transplantation is limited by both their poor proliferation and their differentiation capabilities. Previous studies have shown that microRNAs (miRNA) act as essential mediators in the fate determination of stem/progenitor cells. In this study, we hypothesized that miR-124-3p plays a regulatory role in the fate of RPC determination by targeting Septin10 (SEPT10) in vitro. We observed that the overexpression of miR124-3p downregulates SEPT10 expression in RPCs, leading to reduced RPC proliferation and increased differentiation, specifically towards both neurons and ganglion cells. Conversely, antisense knockdown of miR-124-3p was shown to boost SEPT10 expression, enhance RPC proliferation, and attenuate differentiation. Moreover, overexpression of SEPT10 rescued miR-124-3p-caused proliferation deficiency while weakening the enhancement of miR-124-3p-induced-RPC differentiation. Results from this study show that miR-124-3p regulates RPC proliferation and differentiation by targeting SEPT10. Furthermore, our findings enable a more comprehensive understanding into the mechanisms of proliferation and differentiation of RPC fate determination. Ultimately, this study may be useful for helping researchers and clinicians to develop more promising and effective approaches to optimize the use of RPCs in treating retinal degeneration diseases.
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页码:689 / 704
页数:15
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