Carvedilol Reduces the Neuronal Apoptosis after Ischemic Stroke by Modulating Activator of Transcription 3 Expression in vitro.

IF 2.3 4区 医学 Q2 DEVELOPMENTAL BIOLOGY Developmental Neuroscience Pub Date : 2023-01-01 DOI:10.1159/000527484
Zhao Zheng, Fei Hou, Guodong He, Fengfeng Jiang, Xiang Bao, Minfeng Tong
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Abstract

Cerebral ischemia is divided into local cerebral ischemia and diffuse cerebral ischemia. The etiology of localized cerebral ischemia includes middle cerebral artery embolism; stenosis, occlusion, or thrombosis of extracranial internal carotid artery or vertebral artery; and cerebral artery spasm. The causes of diffuse cerebral ischemia include cardiac arrest, hypotension, anemia, and hypoglycemia. However, the underlying mechanism is still unclear. In this study, we demonstrated that activator of transcription 3 (ATF3) is a hubgene in IS by bioinformatics analysis. The expression of ATF3 was increased in PC12 cells with oxygen-glucose deprivation/reoxygenation (OGD/R) treatment. ATF3 deficiency inhibited cell viability and induced cell apoptosis, whereas ATF3 overexpression showed the opposite role in cell viability and cell apoptosis. Moreover, Carvedilol as a compound targeting ATF3 also facilitated cell viability and reduced cell apoptosis. ATF3 deficiency retarded the increase in cell viability and inhibition of cell apoptosis in OGD/R-PC12 cells with Carvedilol treatment. Additionally, the decreased Bax and cleaved caspase-3 were released in OGD/R-PC12 cells with Carvedilol and siATF3 treatment, while Bcl-2 expression was inhibited in OGD/R-PC12 cells with Carvedilol and siATF3 treatment. In conclusion, Carvedilol may be a key compound targeting ATF3 in OGD/R-PC12 cells. Graphical Abstract: Carvedilol positively regulated cell viability and negatively regulated cell apoptosis in OGD/R-PC12 cells by inhibition of ATF3.

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卡维地洛通过调控转录激活因子3的表达减少缺血性脑卒中后神经元的凋亡。
脑缺血分为局部脑缺血和弥漫性脑缺血。局部脑缺血的病因包括大脑中动脉栓塞;颅内外颈内动脉或椎动脉狭窄、闭塞或血栓形成;还有脑动脉痉挛。引起弥漫性脑缺血的原因包括心脏骤停、低血压、贫血和低血糖。然而,其潜在机制尚不清楚。在本研究中,我们通过生物信息学分析证明了转录激活因子3 (activator of transcription, ATF3)是is中的一个hubgene。在氧-糖剥夺/再氧(OGD/R)处理的PC12细胞中,ATF3的表达增加。ATF3缺乏抑制细胞活力,诱导细胞凋亡,而ATF3过表达对细胞活力和细胞凋亡的作用相反。此外,卡维地洛作为靶向ATF3的化合物也能促进细胞活力,减少细胞凋亡。ATF3缺乏延缓了卡维地洛处理OGD/R-PC12细胞活力的增加和细胞凋亡的抑制。此外,卡维地洛和siATF3在OGD/R-PC12细胞中减少了Bax和裂解的caspase-3的释放,而卡维地洛和siATF3在OGD/R-PC12细胞中抑制了Bcl-2的表达。综上所述,卡维地洛可能是OGD/R-PC12细胞中靶向ATF3的关键化合物。摘要:卡维地洛通过抑制ATF3正向调节OGD/R-PC12细胞活力,负向调节细胞凋亡。
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来源期刊
Developmental Neuroscience
Developmental Neuroscience 医学-发育生物学
CiteScore
4.00
自引率
3.40%
发文量
49
审稿时长
>12 weeks
期刊介绍: ''Developmental Neuroscience'' is a multidisciplinary journal publishing papers covering all stages of invertebrate, vertebrate and human brain development. Emphasis is placed on publishing fundamental as well as translational studies that contribute to our understanding of mechanisms of normal development as well as genetic and environmental causes of abnormal brain development. The journal thus provides valuable information for both physicians and biologists. To meet the rapidly expanding information needs of its readers, the journal combines original papers that report on progress and advances in developmental neuroscience with concise mini-reviews that provide a timely overview of key topics, new insights and ongoing controversies. The editorial standards of ''Developmental Neuroscience'' are high. We are committed to publishing only high quality, complete papers that make significant contributions to the field.
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