冠状动脉微血管疾病中西医研究现状

冠状动脉微血管疾病(coronary microvascular disease,CMVD)是指由于冠状动脉微血管功能和(或)结构异常造成的心肌供血不足及心肌血流量的调节失常,从而引起一系列心肌缺血主观症状和(或)客观依据的一类疾病[1]。既往微血管性心绞痛的的诊断前提为患者无阻塞性冠状动脉疾病,但随着研究的深入发现,阻塞性冠状动脉疾病、冠状动脉血管重建或心脏移植后的患者亦可出现冠状动脉微血管障碍.

人参皂苷Re对氧化低密度脂蛋白诱导的人脐静脉内皮细胞MEK/ERK/NF-κB信号通路的影响

目的基于丝裂原活化蛋白激酶/细胞外调节蛋白激酶/核因子-κB(MEK/ERK/NF-κB)信号通路探讨人参皂苷Re(G-Re)对氧化低密度脂蛋白(ox-LDL)诱导的人脐静脉内皮细胞(HUVECs)炎症反应的影响。方法体外培养HUVECs,分别设置空白对照组、模型组(ox-LDL 150μg/mL)、G-Re组(20μmol/L)、G-Re加MEK抑制剂组(G-Re 20μmol/L+U0126-EtOH 10μmol/L)。采用CCK8法检测细胞活力;ELISA检测细胞上清液炎症因子IL-6和TNF-α表达水平;免疫荧光检测NF-κB蛋白的荧光强度;Western Blot和RT-PCR检测MEK、ERK和NF-κB蛋白和基因表达。结果与空白对照组比较,模型组细胞活力减弱(P<0.01),炎症因子IL-6和TNF-α表达升高(P<0.05),NF-κB蛋白的荧光强度增加(P<0.05),MEK、ERK和NF-κB蛋白及基因表达上调(P<0.05,P<0.01)。与模型组比较,G-Re组干预后细胞活力增强(P<0.05,P<0.01),炎症因子IL-6和TNF-α表达下降(P<0.05,P<0.01),NF-κB蛋白的荧光强度降低(P<0.05),MEK、ERK和NF-κB蛋白及基因表达下调(P<0.05,P<0.01)。与G-Re组比较,G-Re加MEK抑制剂组ERK和NF-κB基因和蛋白表达上调(P<0.05,P<0.01)。结论G-Re能够减轻ox-LDL诱导的HUVECs的炎症反应和内皮损伤,其作用机制可能与抑制MEK/ERK/NF-κB信号通路的激活有关。

宽胸气雾剂治疗冠状动脉微血管疾病典型病例1例

近年来研究发现,因心绞痛接受冠状动脉造影检查的患者中,约50%的患者实际并不存在心外膜冠状动脉阻塞病变[1],这类有心肌缺血主观或客观证据,但冠脉造影检查无异常的疾病即为冠状动脉微血管疾病(coronary microvascular disease,CMVD),它是在多种致病因素的作用下,冠状前小动脉和小动脉的结构和(或)功能异常所致的劳力性心绞痛或心肌缺血客观证据的临床综合征。近年来,随着微血管功能评价技术的完善,CMVD的检出率亦较前提高,但其病理生理机制至今尚无定论,缺乏客观、有效的治疗策略。

Lingbao Huxin Pill Alleviates Apoptosis and Inflammation at Infarct Border Zone through SIRT1-Mediated FOXO1 and NF-κB Pathways in Rat Model of Acute Myocardial Infarction

Objective To investigate whether Lingbao Huxin Pill(LBHX)protects against acute myocardial infarction(AMI)at the infarct border zone(IBZ)of myocardial tissue by regulating apoptosis and inflammation through the sirtuin 1(SIRT1)-mediated forkhead box protein O1(FOXO1)and nuclear factor-κB(NF-κB)signaling pathways.Methods Six-week-old Wistar rats with normal diet were randomized into the sham,the model,Betaloc(0.9 mg/kg daily),LBHX-L(0.45 mg/kg daily),LBHX-M(0.9 mg/kg daily),LBHX-H(1.8 mg/kg daily),and LBHX+EX527(0.9 mg/kg daily)groups according to the method of random number table,13 in each group.In this study,left anterior descending coronary artery(LADCA)ligation was performed to induce an AMI model in rats.The myocardial infarction area was examined using a 2,3,5-triphenyltetrazolium chloride solution staining assay.A TdT-mediated dUTP nick-end labeling(TUNEL)assay was conducted to assess cardiomyocyte apoptosis in the IBZ.The histopathology of myocardial tissue at the IBZ was assessed with Heidenhain,Masson and hematoxylineosin(HE)staining assays.The expression levels of tumor necrosis factorα(TNF-α),interleukin(IL)-6,IL-1β,and intercellular adhesion molecule-1 were measured using enzyme-linked immunosorbent assays(ELISAs).The mRNA expressions of SIRT1 and FOXO1 were detected by real-time qPCR(RT-qPCR).The protein expressions of SIRT1,FOXO1,SOD2,BAX and NF-κB p65 were detected by Western blot analysis.Results The ligation of the LADCA successfully induced an AMI model.The LBHX pretreatment reduced the infarct size in the AMI rats(P<0.01).The TUNEL assay revealed that LBHX inhibited cardiomyocyte apoptosis at the IBZ.Further,the histological examination showed that the LBHX pretreatment decreased the ischemic area of myocardial tissue(P<0.05),myocardial interstitial collagen deposition(P<0.05)and inflammation at the IBZ.The ELISA results indicated that LBHX decreased the serum levels of inflammatory cytokines in the AMI rats(P<0.05 or P<0.01).Furthermore,Western blot analysis revealed that the LBHX pretreatment upregulated the protein levels of SIRT1,FOXO1 and SOD2(P<0.05)and downregulated NF-κB p65 and BAX expressions(P<0.05).The RT-qPCR results showed that LBHX increased the SIRT1 mRNA and FOXO1 mRNA levels(P<0.05).These protective effects,including inhibiting apoptosis and alleviating inflammation in the IBZ,were partially abolished by EX527,an inhibitor of SIRT1.Conclusion LBHX could protect against AMI by suppressing apoptosis and inflammation in AMI rats and the SIRT1-mediated FOXO1 and NF-κB signaling pathways were involved in the cardioprotection effect of LBHX.