机构:[1]Hebei Univ Chinese Med, Grad Sch, Shijiazhuang 050090, Hebei, Peoples R China[2]Hebei Med Univ, Grad Sch, Shijiazhuang 050017, Hebei, Peoples R China[3]Key Lab State Adm Tradit Chinese Med Cardiocerebr, Shijiazhuang 050035, Hebei, Peoples R China[4]Hebei Yiling Pharmaceut Res Inst, Shijiazhuang 050035, Hebei, Peoples R China[5]State Key Lab Collateral Dis Res & Innovat Med, Shijiazhuang 050035, Hebei, Peoples R China[6]Hebei Univ Chinese Med, Affiliated Yiling Hosp, Dept Cardiol, Shijiazhuang 050091, Hebei, Peoples R China
Endothelial-to-mesenchymal transition (EndMT) is an essential mechanism in myocardial fibrosis (MF). Tongxinluo (TXL) has been confirmed to protect the endothelium against reperfusion injury after acutemyocardial infarction (AMI). However, whether TXL can inhibit MF after AMI via inhibiting EndMT remained unknown. This study aims to identify the role of EndMT in MF after AMI as well as the protective effects and underlying mechanisms of TXL on MF. The AMI model was established in rats by ligating left anterior descending coronary artery. Then, rats were administered with high- (0.8 g.kg(-1).d(-1)), mid- (0.4 g.kg(-1).d(-1)), and low- (0.2 g.kg(-1).d(-1)) dose Tongxinluo and benazepril for 4 weeks, respectively. Cardiac function, infarct size, MF, and related indicators of EndMT were measured. In vitro, human cardiac microvascular endothelial cells (HCMECs) were pretreated with TXL for 4 h and then incubated in hypoxia conditions for 3 days to induce EndMT. Under this hypoxic condition, neuregulin-1 (NRG-1) siRNA were further applied to silence NRG-1 expression. Immunofluorescencemicroscopy was used to assess expression of endothelial marker of vWF and fibrotic marker of Vimentin. Related factors of EndMT were determined by Western blot analysis. TXL treatment significantly improved cardiac function, ameliorated MF, reduced collagen of fibrosis area (types I and III collagen) and limited excessive extracellular matrix deposition (mmp2 and mmp9). In addition, TXL inhibited EndMT in cardiac tissue and hypoxia-induced HCMECs. In hypoxia-induced HCMECs, TXL increased the expression of endothelial markers, whereas decreasing the expression of fibrotic markers, partially through enhanced expressions of NRG-1, phosphorylation of ErbB2, ErbB4, AKT, and downregulated expressions of hypoxia inducible factor-1a and transcription factor snail. After NRG-1 knockdown, the protective effect of TXL on HCMEC was partially abolished. In conclusion, TXL attenuates MF after AMI by inhibiting EndMT and through activating the NRG-1/ErbB- PI3K/AKT signalling cascade.
基金:
National Key Research and Development Program [2017YFC1700500]; Hebei Province Natural Science Foundation [H2018106043]; Hebei University of Chinese medicine [CXZZBS2018153]
语种:
外文
被引次数:
WOS:
PubmedID:
中科院(CAS)分区:
出版当年[2020]版:
大类|3 区生物
小类|3 区生物工程与应用微生物4 区医学:研究与实验
最新[2025]版:
大类|4 区医学
小类|4 区生物工程与应用微生物4 区医学:研究与实验
JCR分区:
出版当年[2019]版:
Q3BIOTECHNOLOGY & APPLIED MICROBIOLOGYQ3MEDICINE, RESEARCH & EXPERIMENTAL
最新[2023]版:
Q3BIOTECHNOLOGY & APPLIED MICROBIOLOGYQ3MEDICINE, RESEARCH & EXPERIMENTAL
第一作者机构:[1]Hebei Univ Chinese Med, Grad Sch, Shijiazhuang 050090, Hebei, Peoples R China
通讯作者:
通讯机构:[1]Hebei Univ Chinese Med, Grad Sch, Shijiazhuang 050090, Hebei, Peoples R China[6]Hebei Univ Chinese Med, Affiliated Yiling Hosp, Dept Cardiol, Shijiazhuang 050091, Hebei, Peoples R China
推荐引用方式(GB/T 7714):
Yin Yujie,Zhang Qian,Zhao Qifei,et al.Tongxinluo Attenuates Myocardiac Fibrosis after Acute Myocardial Infarction in Rats via Inhibition of Endothelial-to-Mesenchymal Transition[J].BIOMED RESEARCH INTERNATIONAL.2019,2019:doi:10.1155/2019/6595437.
APA:
Yin, Yujie,Zhang, Qian,Zhao, Qifei,Ding, Guoyuan,Wei, Cong...&Jia, Zhenhua.(2019).Tongxinluo Attenuates Myocardiac Fibrosis after Acute Myocardial Infarction in Rats via Inhibition of Endothelial-to-Mesenchymal Transition.BIOMED RESEARCH INTERNATIONAL,2019,
MLA:
Yin, Yujie,et al."Tongxinluo Attenuates Myocardiac Fibrosis after Acute Myocardial Infarction in Rats via Inhibition of Endothelial-to-Mesenchymal Transition".BIOMED RESEARCH INTERNATIONAL 2019.(2019)
