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辛伐他汀早期干预能更有效抑制压力负荷高血压大鼠心肌肥厚
引用本文:尚福军,王捷频,郑强荪,刘雄涛,薛玉生,李军,赵连友. 辛伐他汀早期干预能更有效抑制压力负荷高血压大鼠心肌肥厚[J]. 心脏杂志, 2011, 23(2): 151-155
作者姓名:尚福军  王捷频  郑强荪  刘雄涛  薛玉生  李军  赵连友
作者单位:1.第四军医大学:1.唐都医院心脏内科,2.药学系药物研究所,陕西 西安 710032
基金项目:国家十一五科技支撑计划高血压综合防治研究子课题项目资助(2006BAI01A03)
摘    要:目的:比较辛伐他汀早期干预与晚期干预对高血压心肌肥厚的防治效果,并初步探讨其机制.方法:采用腹主动脉缩窄法建立压力负荷高血压大鼠模型,在心肌肥厚形成的不同阶段分别给予辛伐他汀[10 mg/(kg·d),ig]干预.采用天狼猩红染色、血流动力学测定等方法,观察和比较辛伐他汀对高血压心肌肥厚和心功能的影响.应用ELISA法...

关 键 词:辛伐他汀  高血压  心肌肥厚  药物干预
收稿时间:2010-05-11

Early intervention with simvastatin exerts improved effects on cardiac hypertrophy in pressure-overload rats than late intervention
SHANG Fu-jun,WANG Jie-pin,ZHENG Qiang-sun,LIU Xiong-tao,XUE Yu-sheng,LI Jun,ZHAO Lian-you. Early intervention with simvastatin exerts improved effects on cardiac hypertrophy in pressure-overload rats than late intervention[J]. Chinese Heart Journal, 2011, 23(2): 151-155
Authors:SHANG Fu-jun  WANG Jie-pin  ZHENG Qiang-sun  LIU Xiong-tao  XUE Yu-sheng  LI Jun  ZHAO Lian-you
Affiliation:SHANG Fu-jun1,WANG Jie-pin2,ZHENG Qiang-sun1,LIU Xiong-tao1,XUE Yu-sheng1,LI Jun1,ZHAO Lian-you1(1.Department of Cardiology,Tangdu Hospital,Xi'an 710038,Shaanxi,China,2.Institute of Materia Medica,School of Pharmacy,Fourth Military Medical University,Xi'an 710032,China)
Abstract:AIM: To compare the effects of early and late intervention with simvastatin on cardiac hypertrophy and to investigate the probable molecular mechanisms. METHODS: In pressure-overload rat model induced by abdominal aortic coarctation, simvastatin [10 mg/(kg·day), IG] was administrated at early or late stage and structural and functional changes were observed by histopathology analysis with picrosirius staining and hemodynamic measurement. The expression of TNF-α and IL-6 and IL-10 protein levels were determined by ELISA and the production of reactive oxygen species (ROS). Activity of NAPDH oxidase in myocardium were measured, respectively, by Fenton reaction and by superoxide dismutase inhibitable cytochrome C reduction assay. RESULTS: In rats at 8 weeks after aortic coarctation, the left ventricle weight and collagen volume fraction in myocardium significantly increased and cardiac diastolic function decreased, compared with those in sham-operated rats (P<0.01). Intervention with simvastatin at early and late stages both markedly decreased the left ventricle weight and collagen volume fraction (P<0.05). However, left ventricle weight and collagen volume fraction in early intervention group were lower than those in late intervention group (P<0.05). The early intervention also improved the diastolic function and the contents of TNF-α and IL-6. ROS production and NADPH oxidase activity in myocardium were all elevated in pressure-overload rats, which were attenuated by simvastatin intervention at both stages. Contents of TNF-α and IL-6, production of ROS, and activity of NADPH oxidase in rats in early intervention group were lower than those in late intervention group (P<0.05). CONCLUSION: The effects of early intervention with simvastatin on cardiac hypertrophy in pressure-overload rats are superior to those of late intervention, which is probably attributed to the stronger inhibitory effects of early intervention with simvastatin on the expression of proinflammatory cytokines and production of ROS.
Keywords:simvastatin  hypertension  cardiac hypertrophy  medical intervention  
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