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基质金属蛋白酶9在大鼠单纯收缩期高血压模型发生中的作用
引用本文:雷梦觉,朱光照,陈慰云,艾文伟,邬 甦,吴克琴. 基质金属蛋白酶9在大鼠单纯收缩期高血压模型发生中的作用[J]. 中华老年多器官疾病杂志, 2012, 11(1): 58-64
作者姓名:雷梦觉  朱光照  陈慰云  艾文伟  邬 甦  吴克琴
作者单位:1. 江西省人民医院干部心内二科江西省心血管病研究所江西省老年医学研究所,南昌,330006
2. 江西省新余市人民医院心内科,新余,330046
3. 南昌大学医学院基础部,南昌,330008
基金项目:江西省卫生厅重大攻关课题
摘    要:目的 研究基质金属蛋白酶9(MMP-9)在单纯收缩期高血压形成中的作用.方法 选用8周龄Wistar 雄性大鼠20只作为研究对象,随机分成两组,模型组(n=10)和对照组(n=10).应用华法林和维生素K1诱导动脉中层钙化,8周后右侧颈动脉插管进行有创血压和心室内压力的检测.以及取材主动脉,Von Kossa染色分析动脉钙化程度;采用原子吸收光谱法测定血管组织中钙含量.采用弹性纤维染色法观察主动脉组织中弹性纤维形状;应用免疫组织化学和Western blot检测主动脉组织中MMP-9的表达水平.结果 模型组大鼠血压与对照组相比明显增高[收缩压:( 151±9) vs (113±7) mmHg,P<0.01,舒张压:(122±10) vs (98±8) mmHg,P<0.05];而各组间平均左室内压无明显变化.模型组大鼠血压变化的同时伴有动脉形态结构的改变,主动脉和颈动脉中层钙化明显,模型组主动脉钙含量明显高于对照组[(17.9±1.8)vs(5.8±0.6)mg/g,P<0.01].弹力纤维断裂变直,失去波浪形状.Western免疫印迹法分析模型组MMP-9蛋白表达较对照组明显升高.结论 利用华法林和维生素K1诱导的单纯收缩期高血压大鼠是可重复性好,便捷,以及与人体衰老相似较为理想的模型.MMP-9酶表达明显增多可促使大动脉中层弹力蛋白降解和钙在弹力纤维薄层的沉积,从而在单纯收缩期高血压形成中发挥着一定作用.

关 键 词:大鼠  单纯收缩期高血压  动脉钙化  基质金属蛋白酶9

Matrix metalloproteinase-9 in rat model of isolated systolic hypertension
LEI Mengjue,ZHU Guangzhao,CHEN Weiyun,et al. Matrix metalloproteinase-9 in rat model of isolated systolic hypertension[J]. Chinese Journal of Multiple Organ Diseases in the Elderly, 2012, 11(1): 58-64
Authors:LEI Mengjue  ZHU Guangzhao  CHEN Weiyun  et al
Affiliation:1 Department of Geriatirc Cardiology, Jiangxi Provincial People's Hospital, Nanchang 330006, China; 2Department of Cardiology Jiangxi Provinvial Xinyu Municipal People's Hospital, Xinyu 330046, China; 3Department of Basic Medicine, Medical College Nanchang University, Nanchang 330008, China)
Abstract:Objective To investigate the role of matrix metalloproteinase-9(MMP-9) in the formation of isolated systolic hypertension so as to provide a new model of isolated systolic hypertension. Methods Twenty 8-week old male Wistar rats were randomly divided into the model group (n=10) and control group(n=10). To induce large artery calcification, rats were treated with warfarin and vitamin KI. Eight weeks later, blood pressure and left ventricular pressure were measured by right carotid arterial cannulation. The segments from each aorta were processed for histological analysis by Von Kossa methed. Aortic calcium contents were calculated in each group with atom-spectrum. Elastic fiber structure in aorta was analyzed by elastic fiber staining. MMP-9 expression was determined by immunohistochemistry and Western blot. Results Compared with control group, blood pressures were significantly higher in model group[systolic blood pressure: (151 ±9) vs (113 ±7)mmHg, P〈0.01; diastolic blood pressure: (122± 10) vs (98 ± 8)mmHg, P〈0.05]. The mean left ventricular pressure was not significantly different between the two groups. In model group, the blood pressure fluctuation was associated with morphological change of the aorta, such as extensive arterial medial elastocalcinosis. Compared with control group, calcium content in aorta was significantly higher in model group [(17.9 ± 1.8) vs (5.8 ± 0.6)mg/g, P 〈 0.01]; the elastic lamellae was flatten and lost natural waviness. Western blot analysis showed that MMP-9 protein expression level was significantly higher in model group than in control group. Conclusion Chronic treatment with warfarin and vitamin K1 produce a satisfactory model of isolated systolic hypertension which is identical to the disorder in humans. The elevated expression of MMP-9 enhances the elastin degeneration and calcification of the aortic elastic fibers and plays a role in the formation of isolated systolic hypertension.
Keywords:rats  vascular calcification  matrix metalloproteinase 9
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