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Dynamic changes in myocardial matrix metalloproteinase activity in mice with viral myocarditis

机译:病毒性心肌炎小鼠心肌基质金属蛋白酶活性的动态变化

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Background Matrix metalloproteinases (MMPs) are the major regulators of collagen degradation involved in the pathogenesis of several diseases of the heart. The purpose of this study was to investigate the dynamic changes in myocardial MMP activity in mice with viral myocarditis (VM), the relationship between MMP activity and both cardiac function and the quantity of myocardial collagen, and the role MMPs playing in the pathological lesions of VM. Methods Sixty-five six-week-old male DBA/2 mice were divided into two groups. Mice in the infected group (n =50) were inoculated intraperitoneally with 0.14 ml of Coxsackievirus B_3(CVB_3, Nancy strain). Control mice (n =15) were inoculated intraperitoneally with 0.14 ml of Eagle' s medium. Eight infected mice and three control mice were sacrificed on each of days 3, 7, 10, 21 and 30 after inoculation. MMP activity was measured on an SDS-PAGE substrate gel embedded with type Ⅰ gelatin ( zymography) . Echocardiographic studies were performed under anesthesia with 3% chloralhydrate administered intraperitoneally (0.01 ml/g - 0.015 ml/g). Cardiac systolic function indices, such as peak velocity of the aorta (V_p), flow velocity integral of the aorta (V_i), ejection fraction (EF), and fractional shortening (FS) were determined by echocardiography. Histological cross sections of the hearts were stained with hematoxylin-eosin and myocardial histopathological scores were determined under an optical microscope. The amount of myocardial collagen was measured by means of hydroxyproline quantification. Results In virus-infected mice, both MMP-2 and MMP-9 activities were significantly higher than in control mice, reaching a peak on day 10 (P < 0. 01). On day 10, cardiac systolic function indices (EF, FS, V_p, and V_i) were all significantly lower compared both to other stages following viral inoculation and to the control group (P < 0. 05). In the acute stage, the amount of myocardial collagen in mice with VM was not significantly different from normal control mice (P > 0. 05). However, the amount of myocardial collagen in infected mice at the recovery stage (on days 21 and 30) was significantly greater than those of the control mice. MMP-2 and MMP-9 activities positively correlated with myocardial histopathological scores (r = 0. 801,0. 821, P < 0. 01) and negatively correlated with V_p(r= - 0.649, -0.683, P < 0. 01) and V_i ( r = -0. 711, -0.755, P < 0. 01). However, V_p negatively correlated with myocardial histopathological scores (r= -0. 756, P < 0. 01). Conclusions In mice with VM, the activities of myocardial MMP-2 and MMP-9 increase significantly during the acute stage, and the total quantity of myocardial collagen increases by the time of recovery. These changes are associated with myocardial interstition remodeling and cardiac dysfunction. MMP activity is an important reference marker for myocardial pathological lesions and can be used to evaluate the severity of myocardial interstitial damage and cardiac dysfunction.
机译:背景技术基质金属蛋白酶(MMP)是胶原降解的主要调节剂,参与心脏几种疾病的发病机制。这项研究的目的是调查病毒性心肌炎(VM)小鼠心肌MMP活性的动态变化,MMP活性与心脏功能和心肌胶原数量之间的关系,以及MMP在小鼠病理性病变中的作用虚拟机。方法将65只6周龄的雄性DBA / 2小鼠分为两组。感染组(n = 50)的小鼠腹腔内接种0.14 ml柯萨奇病毒B_3(CVB_3,南希病毒株)。对照小鼠(n = 15)被腹膜内接种0.14ml的Eagle氏培养基。接种后第3、7、10、21和30天每天处死八只感染小鼠和三只对照小鼠。在包埋有Ⅰ型明胶的SDS-PAGE底物凝胶上测定MMP活性(酶谱法)。超声检查是在麻醉下腹膜内给予3%的水合氯醛(0.01 ml / g-0.015 ml / g)进行的。通过超声心动图确定心脏的收缩功能指标,例如主动脉的峰值速度(V_p),主动脉的流速积分(V_i),射血分数(EF)和缩短分数(FS)。用苏木精-曙红对心脏的组织学切片进行染色,并在光学显微镜下测定心肌的组织病理学评分。通过羟脯氨酸定量测量心肌胶原的量。结果在病毒感染的小鼠中,MMP-2和MMP-9活性均显着高于对照小鼠,并在第10天达到峰值(P <0. 01)。在第10天,与病毒接种后的其他阶段和对照组相比,心脏的收缩功能指数(EF,FS,V_p和V_i)均显着降低(P <0. 05)。在急性期,VM小鼠的心肌胶原蛋白含量与正常对照组相比无显着差异(P> 0. 05)。但是,在恢复阶段(第21天和第30天)感染小鼠的心肌胶原蛋白的量显着大于对照小鼠。 MMP-2和MMP-9活性与心肌组织病理学评分呈正相关(r = 0. 801,0。821,P <0. 01),与V_p呈负相关(r =-0.649,-0.683,P <0. 01 )和V_i(r = -0。711,-0.755,P <0.01)。但是,V_p与心肌组织病理学评分呈负相关(r = -0。756,P <0. 01)。结论VM小鼠在急性期心肌MMP-2和MMP-9的活性显着增加,恢复时心肌胶原的总量增加。这些变化与心肌间质重塑和心脏功能障碍有关。 MMP活性是心肌病理损伤的重要参考标记,可用于评估心肌间质损害和心脏功能障碍的严重程度。

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