齐墩果酸通过抑制miR-186-5p表达抑制缺血性脑卒中神经元焦亡。

IF 1.8 4区 医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL
Shi-Chang Cai, Xiu-Ping Li, Xing Li, Gen-Yun Tang, Li-Ming Yi, Xiang-Shang Hu
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引用次数: 2

摘要

缺血性中风是导致人类残疾和死亡的常见疾病。既往研究表明齐墩果酸(OA)可改善氧化损伤和脑缺血损伤,并证实缺血脑卒中患者血清中miR-186-5p升高。在此,我们研究OA是否通过调节miR-186-5p的表达来控制神经球蛋白(Ngb)的水平,从而抑制缺血性脑卒中中的神经元焦亡。将3种浓度的OA(0.5、2、8 μM)分别加入缺血脑卒中细胞模型海马原代神经元中。我们发现OA治疗明显抑制焦亡。qRT-PCR和western blot结果显示,OA抑制了焦热相关基因的表达。此外,OA抑制LDH和促炎细胞因子的释放。此外,在oa处理的OGD/R神经元中,miR-186-5p下调,Ngb上调。MiR-186-5p敲低抑制OGD/ r诱导的焦亡,抑制LDH和炎症细胞因子释放。此外,双荧光素酶报告试验证实miR-186-5p直接靶向Ngb。OA降低miR-186-5p以调节Ngb水平,从而抑制OGD/ r处理的神经元和MCAO小鼠的焦亡。综上所述,OA通过下调miR-186-5p和上调Ngb表达,在体内外均可减轻焦亡,这为OA可作为缺血性脑卒中的药物提供了新的理论依据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Oleanolic Acid Inhibits Neuronal Pyroptosis in Ischaemic Stroke by Inhibiting miR-186-5p Expression.

Oleanolic Acid Inhibits Neuronal Pyroptosis in Ischaemic Stroke by Inhibiting miR-186-5p Expression.

Oleanolic Acid Inhibits Neuronal Pyroptosis in Ischaemic Stroke by Inhibiting miR-186-5p Expression.

Oleanolic Acid Inhibits Neuronal Pyroptosis in Ischaemic Stroke by Inhibiting miR-186-5p Expression.

Ischaemic stroke is a common condition leading to human disability and death. Previous studies have shown that oleanolic acid (OA) ameliorates oxidative injury and cerebral ischaemic damage, and miR-186-5p is verified to be elevated in serum from ischaemic stroke patients. Herein, we investigated whether OA regulates miR-186-5p expression to control neuroglobin (Ngb) levels, thereby inhibiting neuronal pyroptosis in ischaemic stroke. Three concentrations of OA (0.5, 2, or 8 μM) were added to primary hippocampal neurons subjected to oxygen-glucose deprivation/reperfusion (OGD/R), a cell model of ischaemic stroke. We found that OA treatment markedly inhibited pyroptosis. qRT-PCR and western blot revealed that OA suppressed the expression of pyroptosis-associated genes. Furthermore, OA inhibited LDH and proinflammatory cytokine release. In addition, miR-186-5p was downregulated while Ngb was upregulated in OA-treated OGD/R neurons. MiR-186-5p knockdown repressed OGD/R-induced pyroptosis and suppressed LDH and inflammatory cytokine release. In addition, a dual luciferase reporter assay confirmed that miR-186-5p directly targeted Ngb. OA reduced miR-186-5p to regulate Ngb levels, thereby inhibiting pyroptosis in both OGD/R-treated neurons and MCAO mice. In conclusion, OA alleviates pyroptosis in vivo and in vitro by downregulating miR-186-5p and upregulating Ngb expression, which provides a novel theoretical basis illustrating that OA can be considered a drug for ischaemic stroke.

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来源期刊
Experimental Neurobiology
Experimental Neurobiology Neuroscience-Cellular and Molecular Neuroscience
CiteScore
4.30
自引率
4.20%
发文量
29
期刊介绍: Experimental Neurobiology is an international forum for interdisciplinary investigations of the nervous system. The journal aims to publish papers that present novel observations in all fields of neuroscience, encompassing cellular & molecular neuroscience, development/differentiation/plasticity, neurobiology of disease, systems/cognitive/behavioral neuroscience, drug development & industrial application, brain-machine interface, methodologies/tools, and clinical neuroscience. It should be of interest to a broad scientific audience working on the biochemical, molecular biological, cell biological, pharmacological, physiological, psychophysical, clinical, anatomical, cognitive, and biotechnological aspects of neuroscience. The journal publishes both original research articles and review articles. Experimental Neurobiology is an open access, peer-reviewed online journal. The journal is published jointly by The Korean Society for Brain and Neural Sciences & The Korean Society for Neurodegenerative Disease.
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