黄芪多糖通过调节Drp1介导的线粒体分裂改善感染性心肌病

目的从线粒体动力相关蛋白1(Dp1)介导线粒体分裂平衡角度,解读黄芪多糖(APS)对感染性心肌病小鼠的心功能保护作用及机制。方法按随机数字表法将18只成年雄性C57BL/6J小鼠分为对照组、脂多糖(LPS)组和LPS+APS组,每组6只。采用LPS诱导制备感染性:心肌病模型。各组均于术后6h经尾静脉取外周血,采用酶联免疫吸附试验(ELISA)检测小鼠血清炎性因子水平;LPS处理后24 h行超声心动图检查心室功能,包括左室射血分数(LVEF)、左室短轴缩短率(LVFS)、左室舒张期末内径(LVEDD)和左室收缩期末内径(LVESD);检查后即刻处死小鼠取心肌组织,采用蛋白质印迹试验(Western bloting)检测肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)、C3a、Drp1、线粒体分裂蛋白1(Fis1)、线粒体融合蛋白2(Mfn2)、视神经菱缩蛋白1(Opa1)蛋白表达。将购买的小鼠心房肌细胞株HL-1分为对照组、LPS组、LPS+APS组和LPS+APS+线粒体氧化磷酸化解偶联剂(FCCP)组。采用活性氧(ROS)检测试剂盒检测分离线粒体及HL-1细胞内的ROS含量:采用线粒体膜电位检测试剂盒(JC-1)检测线粒体膜电位(MMP);采用三磷酸腺背(ATP)检测试剂盒检测HL-1细胞内ATP含量。结果与对照组比较.LPS组小鼠心脏的LVEF、LNFS、LVEDD和LVESD均明显降低.线粒体内ROS含量明显升高,MMP和ATP含量均明显下降;而APS可改善感染性心肌病小鼠的心功能指标[LVEF:0.571±0.026比0.287±0.045.LVFS(%):33.13±2.11比21.22±0.99.LVEDD(mm):3.74±0.10比2.77±0.05.LVESD(mm):2.74±0.09比1.99±0.04.均P<0.05].明显降低心肌内ROS含量[ROS(%):138.39±9.28比260.97±19.22.P<0.05].明显抑制MMP和ATP含量下降[MMP(红色1绿色荧光强度比值):0.91±0.05比0.55±0.01,ATP(%):94.22±10.11比58.74±5.39.均P<0.05),且APS可明显抑制LPS处理后的Drp1和Fis1蛋白过表达以及MIn2和Opal蛋白低表达[Drp1/GAPDH(%):126.33±11.70比218.75±19.44,Fis1/CAPDH(%):105.71±15.77比194.39±5.27,Mfn2/CAPDH(%):92.75±10.44比41.88±3.95,0pa1/CAPDH(%):98.14±3.71比55.94±7.30.均P<0.05]。故进一步采用HL-1细胞构建感染性心肌病模型,HL-1细胞经FCCP处理后可明显抑制APS的保护效应。结论APS通过抑制Drp1过表达,抑制线粒体的过度分裂,减轻感染性心肌细胞的氧化应激和线粒体损伤,最终改善心脏功能,该机制的发现可为感染性心肌病的治疗提供新的理论依据和临床参考。

中药治疗病毒性心肌炎的实验研究进展

病毒性心肌炎（vital myocarditis，VMC）是临床最常见的感染性心肌病，患病者主要为青少年和成人，8％-12％会出现猝死现象。柯萨奇病毒主要包括疱疹病毒、肠道病毒、艾巴氏病毒、腺病毒等。

心脏超声与MRI检查在肥厚型心肌病伴感染性心内膜炎的诊断价值比较

目的:比较心脏超声与MRI检查在肥厚型心肌病伴感染性心内膜炎的诊断价值。方法:抽取100例肥厚型心肌病伴感染性心内膜炎患者为研究对象,分别给予超声与MRI诊断。比较超声和MRI检查方式下不同部位的心肌厚度,统计两种检查方式对不同部位的赘生物的检出率和不同大小赘生物的检出率。结果:MRI检查下侧壁和后尖部心肌厚度明显大于超声检查,MRI检查对主动脉瓣、肺动脉瓣赘生物的检出率均明显大于心脏超声,对不同大小赘生物的检出率均明显大于心脏超声,差异均有统计学意义(P<0.05)。结论:MRI检查在肥厚型心肌病伴感染性心内膜炎中的诊断价值高于心脏超声检查。

ROLE OF COXSACKIEVIRUS AND ADENOVIRUS RECEPTOR (CAR)IN CARDIOTOXICITY INFECTED BY COXSACKIEVIRUS B3

Objective To explore the role of coxsackievirus and adenovirus receptor（CAR） in cardiotoxicity infected by coxsackieviras B3. Methods A toxic cellular model was established in vitro by adding myocarditic coxsackievirus B3 （CVB3m） into the culture of neonatal mouse cardiomyocytes. 48 h later, the cardiomyocytes were divided into control, CVB3m, and CAR antibody ＋ CVB3m groups. CVB3m-mediated myocytopathic effect of above three groups was observed after further culturing for 48h. At the same time, the cardiomyocytes＇ viability of above three groups was assessed by MTT assay. Results The degree of cytopathic effect（CPE） of CAR antibody ＋ CVB3m group was significantly lower than CVB3m group （ P 〈 0. 01 ） and there was a significant increase in cell viability in CAR antibody ＋ CVB3m group compared with CVB3m group（ P 〈 0. 01 ）. No significant difference was found between CAR antibody ＋ CVB3m group and control group. Conclusion CAR antibody possesses a protective effect on CVB3m infected cardiomyoctyes, which indicates that CAR may play an important role in mediating cardiotoxicity infected by CVB3m.