| 一氧化氮在铁诱导的大鼠心肌损伤中的作用 |
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| 作者姓名: | Ying-Ying C Qiang X Chun-Mei C Zhi-Guo Y Yue-Liang S Lin-Lin W |
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| 作者单位: | 浙江大学医学院生理教研室,杭州,310031 |
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| 基金项目: | The work was supported by the Natural Science Foundation of Zhejiang for Talents (No. RC99038) and Fund for Outstanding Young Scientists of Zhejiang University School of Medicine. |
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| 摘 要: | 采用Langendorff灌流大鼠心脏和酶解分离的心肌细胞为实验模型,研究铁负荷下心肌损伤情况以及一氧化氮(NO)在铁诱导的心肌损伤中的地位。结果显示:(1)心肌铁负荷(Fe-HQ)可使分离心肌细胞舒张期细胞长度缩短、收缩幅度和速度降低,离体灌流心脏左室发展压(LVDP)、±dp/dtmax、冠脉流量呈现双相变化;冠脉流出液中乳酸脱氢酶(LDH)、肌酸激酶(CK)释放量和心肌丙二醛(MDA)增高。(2)NO的前体L-精氨酸(L-argi-nine,L-Arg)引起心肌细胞舒张期细胞长度缩短、收缩幅度降低。离体灌流心脏LVDP、冠脉流量、和±dp/dtmax增高,用K-H液复灌后可恢复正常。(3)L-Arg预处理,再行Fe-HQ灌流,与单纯的L-Arg或Fe-HQ组相比,心肌细胞舒张期细胞长度、收缩幅度和速度减小;离体灌流心脏LVDP、±dp/dtmax、心率和冠脉流量明显下降,冠脉流出液中LDH、CK增加。(4)Nω-硝基-L-精氨酸甲酯(L-NAME)和Fe-HQ合并灌流后,与单纯Fe-HQ组相比,心肌细胞舒张期细胞长度、收缩幅度和速度增加。L-NAME可阻断Fe-HQ引起的LVDP、左室舒张末压(LVEDP)和±dp/dtmax降低,冠脉流出液中LDH、CK增高。(5)用Triton X-100短暂处理以去除冠脉内皮后,与保留冠脉内皮的心肌相比,Fe-HQ引起的LVDP和±dp/dtmax的一过性增高现象被抑制,但
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| 关 键 词: | 心肌缺血 一氧化氮 铁诱导 大鼠 心肌损伤 |
| 修稿时间: | 2001年12月25 |
Role of nitric oxide in iron-induced toxicity in rat hearts |
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| Ying-Ying C,Qiang X,Chun-Mei C,Zhi-Guo Y,Yue-Liang S,Lin-Lin W.Role of nitric oxide in iron-induced toxicity in rat hearts[J].Acta Physiologica Sinica,2002,54(4):300-306. |
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| Authors: | Ying-Ying Chen Qiang Xia Chun-Mei Cao Zhi-Guo Ye Yue-Liang Shen Lin-Lin Wang |
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| Institution: | Department of Physiology, Zhejiang University School of Medicine, Hangzhou 310031. |
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| Abstract: | The aim of the present study was to explore the effect of nitric oxide (NO) on iron-induced toxicity in rat hearts. Langendorff perfused rat heart and enzymatically isolated cardiomyocytes were used. It was shown that lipophilic Fe-HQ reduced the contractile amplitude, velocity and end-diastolic cell length in the cardiomyocyte, while the left ventricular developed pressure (LVDP), +/-dp/dt(max), heart rate and coronary flow showed biphasic alterations, which increased in the first 2 min and then was followed by a decline in isolated perfused rat heart; the contents of lactate dehydrogenase (LDH) and creatine kinase (CK) in the coronary effluent and the malondialdehyde (MDA) in the myocardium were increased. L-arginine (L-Arg), an NO precursor, reduced the contractile amplitude and end-diastolic cell length in the cardiomyocyte; but reversibly increased LVDP, +/-dp/dt(max), and coronary flow in isolated perfused rat heart. Pretreatment with L-Arg aggravated the Fe-HQ-induced decrease in contractile amplitude, velocity and end-diastolic cell length in the cardiomyocyte; LVDP, +/-dp/dt(max), heart rate and coronary flow were significantly reduced in the perfused heart, and the levels of LDH and CK increased in the coronary effluent. In contrast, the NOS inhibitor N(omega)-nitro-L-arginine methyl ester (L-NAME) blocked the Fe-HQ induced change in contractile amplitude, velocity and end-diastolic cell length in the cardio- myocyte; it inhibited the decrease in LVDP, LVEDP and +/-dp/dt(max), and reduced the LDH and CK. Removing endothelial cells in coronary vessels attenuated the increase in LVDP and +/-dp/dt(max) at the beginning of Fe-HQ perfusion. It is suggested that L-Arg aggravates the iron-induced cardiac dysfunction, NO can mediate the iron-induced toxicity in heart, and endothelial cells in coronary vessels play an important role in the early stage of the effect of iron. |
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| Keywords: | iron heart nitric oxide L-arginine NG-nitroarginine methyl ester |
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