MicroRNA-130a通过靶向XIAP调控缺血性脑卒中大鼠的神经功能缺损和血管生成。

IF 5.3 2区 医学 Q1 Biochemistry, Genetics and Molecular Biology
Journal of Cellular and Molecular Medicine Pub Date : 2020-09-01 Epub Date: 2020-08-13 DOI:10.1111/jcmm.15732
Wenjing Deng, Chenghe Fan, Yanan Zhao, Yuewei Mao, Jiajia Li, Yonggan Zhang, Junfang Teng
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引用次数: 11

摘要

MicroRNAs (miRNAs)已经被认为与缺血性卒中的发展有关。我们旨在研究miR-130a通过调节X-linked inhibitor of apoptosis protein (XIAP)在缺血性脑卒中大鼠神经功能缺损和血管生成中的作用。采用缝合闭塞法建立大脑中动脉闭塞(MCAO)模型,然后用miR-130a模拟物/抑制剂或/和改变的XIAP处理MCAO大鼠,检测MCAO大鼠神经功能、神经损伤和血管生成的变化。建立氧糖剥夺(OGD)细胞模型,分别处理miR-130a和XIAP在神经元活力和凋亡中的作用。检测miR-130a和XIAP在MCAO大鼠脑组织和ogd处理神经元中的表达水平。通过荧光素酶活性测定验证miR-130a与XIAP的结合位点。在MCAO大鼠和ogd处理的神经元中,MiR-130a过表达,而XIAP下调。在动物模型中,抑制miR-130a可改善MCAO大鼠的神经功能,减轻神经损伤,增加脑组织新生血管。在细胞模型中,miR-130a抑制可促进神经元活力并抑制细胞凋亡。抑制XIAP逆转了MCAO大鼠和ogd处理神经元中抑制miR-130a的作用。XIAP被确定为miR-130a的靶标。我们的研究表明,miR-130a通过靶向XIAP调节MCAO大鼠的神经功能缺损和血管生成。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

MicroRNA-130a regulates neurological deficit and angiogenesis in rats with ischaemic stroke by targeting XIAP.

MicroRNA-130a regulates neurological deficit and angiogenesis in rats with ischaemic stroke by targeting XIAP.

MicroRNA-130a regulates neurological deficit and angiogenesis in rats with ischaemic stroke by targeting XIAP.

MicroRNA-130a regulates neurological deficit and angiogenesis in rats with ischaemic stroke by targeting XIAP.

MicroRNAs (miRNAs) have already been proposed to be implicated in the development of ischaemic stroke. We aim to investigate the role of miR-130a in the neurological deficit and angiogenesis in rats with ischaemic stroke by regulating X-linked inhibitor of apoptosis protein (XIAP). Middle cerebral artery occlusion (MCAO) models were established by suture-occluded method, and MCAO rats were then treated with miR-130a mimics/inhibitors or/and altered XIAP for detection of changes of rats' neurological function, nerve damage and angiogenesis in MCAO rats. The oxygen-glucose deprivation (OGD) cellular models were established and respectively treated to determine the roles of miR-130a and XIAP in neuronal viability and apoptosis. The expression levels of miR-130a and XIAP in brain tissues of MCAO rats and OGD-treated neurons were detected. The binding site between miR-130a and XIAP was verified by luciferase activity assay. MiR-130a was overexpressed while XIAP was down-regulated in MCAO rats and OGD-treated neurons. In animal models, suppressed miR-130a improved neurological function, alleviated nerve damage and increased new vessels in brain tissues of rats with MCAO. In cellular models, miR-130a inhibition promoted neuronal viability and suppressed apoptosis. Inhibited XIAP reversed the effect of inhibited miR-130a in both MCAO rats and OGD-treated neurons. XIAP was identified as a target of miR-130a. Our study reveals that miR-130a regulates neurological deficit and angiogenesis in rats with MCAO by targeting XIAP.

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来源期刊
CiteScore
10.00
自引率
1.90%
发文量
496
审稿时长
28 weeks
期刊介绍: Bridging physiology and cellular medicine, and molecular biology and molecular therapeutics, Journal of Cellular and Molecular Medicine publishes basic research that furthers our understanding of the cellular and molecular mechanisms of disease and translational studies that convert this knowledge into therapeutic approaches.
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