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基于神经功能和转录组综合分析揭示圣愈汤治疗缺血性脑卒中的作用机制

Unique mechanisms of sheng yu decoction ( shèng yù tang) on ischemic stroke mice revealed by an integrated neurofunctional and transcriptome analysis.

机构信息

Department of Traditional Medicine, Tao-yuan General Hospital, Department of Health, Tao-yuan, Taiwan. ; Department of Bioscience Technology, Chuan-yuan Christian University, Taoyuan, Taiwan.

Division of Clinical Chinese Medicine, National Research Institute of Chinese Medicine, Taipei, Taiwan.

出版信息

J Tradit Complement Med. 2013 Oct;3(4):240-9. doi: 10.4103/2225-4110.119703.

Abstract

Sheng Yu Decoction ( Shèng Yù Tang; SYD) is a popular traditional Chinese medicine (TCM) remedy used in treating cardiovascular and brain-related dysfunction clinically; yet, its neuroprotective mechanisms are still unclear. Here, mice were subjected to an acute ischemic stroke to examine the efficacy and mechanisms of action of SYD by an integrated neurofunctional and transcriptome analysis. More than 80% of the mice died within 2 days after ischemic stroke with vehicle treatment. Treatments with SYD (1.0 g/kg, twice daily, orally or p.o.) and recombinant thrombolytic tissue plasminogen activator (rt-PA; 10 mg/kg, once daily, intravenously or i.v.) both significantly extended the lifespan as compared to that of the vehicle-treated stroke group. SYD successfully restored brain function, ameliorated cerebral infarction and oxidative stress, and significantly improved neurological deficits in mice with stroke. Molecular impact of SYD by a genome-wide transcriptome analysis using brains from stroke mice showed a total of 162 out of 2081 ischemia-induced probe sets were significantly influenced by SYD. Mining the functional modules and genetic networks of these 162 genes revealed a significant upregulation of neuroprotective genes in Wnt receptor signaling pathway (3 genes) and regulation of cell communication (7 genes) and downregulation of destructive genes in response to stress (13 genes) and in the induction of inflammation (5 genes), cytokine production (4 genes), angiogenesis (3 genes), vasculature (6 genes) and blood vessel (5 genes) development, wound healing (7 genes), defense response (7 genes), chemotaxis (4 genes), immune response (7 genes), antigen processing and presenting (3 genes), and leukocyte-mediated cytotoxicity (2 genes) by SYD. Our results suggest that SYD could protect mice against ischemic stroke primarily through significantly downregulating the damaging genes involved in stress, inflammation, angiogenesis, blood vessel formation, immune responses, and wound healing, as well as upregulating the genes mediating neurogenesis and cell communication, which make SYD beneficial for treating ischemic stroke.

摘要

圣愈汤(SYD)是一种常用于治疗心血管和脑相关功能障碍的中药方剂,但其神经保护机制尚不清楚。在这里,我们通过整合神经功能和转录组分析,在急性缺血性中风小鼠模型中,研究 SYD 的疗效和作用机制。与 vehicle 处理的中风组相比,用 SYD(1.0 g/kg,每日两次,口服或 p.o.)和重组溶栓组织纤溶酶原激活物(rt-PA;10 mg/kg,每日一次,静脉内或 i.v.)治疗的小鼠的存活率显著延长。SYD 成功恢复了中风小鼠的大脑功能,改善了脑梗死和氧化应激,并显著改善了中风小鼠的神经功能缺损。使用中风小鼠的大脑进行全基因组转录组分析,对 SYD 的分子影响显示,2081 个缺血诱导探针中有 162 个被 SYD 显著影响。挖掘这些 162 个基因的功能模块和遗传网络,揭示了 Wnt 受体信号通路(3 个基因)和细胞通讯调节(7 个基因)中神经保护基因的显著上调,以及应激反应(13 个基因)和炎症诱导(5 个基因)、细胞因子产生(4 个基因)、血管生成(3 个基因)、脉管系统(6 个基因)和血管(5 个基因)发育、伤口愈合(7 个基因)、防御反应(7 个基因)、趋化性(4 个基因)、免疫反应(7 个基因)、抗原加工和呈递(3 个基因)和白细胞介导的细胞毒性(2 个基因)中破坏性基因的下调。我们的结果表明,SYD 可能通过显著下调参与应激、炎症、血管生成、血管形成、免疫反应和伤口愈合的破坏性基因,以及上调介导神经发生和细胞通讯的基因,从而保护小鼠免受缺血性中风的影响,这使得 SYD 有益于治疗缺血性中风。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7291/3925003/f0b235a7464f/JTCM-3-240-g001.jpg

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