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Taurine inhibits ischemia/reperfusion-induced compartment syndrome in rabbits
引用本文:Wang JX,Li Y,Zhang LK,Zhao J,Pang YZ,Tang CS,Zhang J. Taurine inhibits ischemia/reperfusion-induced compartment syndrome in rabbits[J]. Acta pharmacologica Sinica, 2005, 26(7): 821-827
作者姓名:Wang JX  Li Y  Zhang LK  Zhao J  Pang YZ  Tang CS  Zhang J
作者单位:[1]InstituteofCardiovascularDiseaseResearch,TheFirstHospitalofPekingUniversity,Beijing100034,China//KeyLaboratoryofMolecularCardiovascularScience,MinistryofEducation,Beijing100083,China [2]InstituteofCardiovascularDiseaseResearch,TheFirstHospitalofPekingUniversity,Beijing100034,China [3]DepartmentofPathophysiology,CapitalInstituteofMedicine,Beijing100054 [4]DepartmentofPhysiology,HealthCenterofMedicalSciences,PekingUniversity,Beijing100083,China [5]KeyLaboratoryofMolecularCardiovascularScience,MinistryofEducation,Beijing100083,China//DepartmentofPhysiology,HealthCenterofMedicalSciences,PekingUniversity,Beijing100083,China
摘    要:

关 键 词:缺氧再灌注损伤    动物实验  氧化损伤  腓肠肌  车厢综合症

Taurine inhibits ischemia/reperfusion-induced compartment syndrome in rabbits
Wang Ji-Xian,Li Yan,Zhang Li-Ke,Zhao Jing,Pang Yong-Zheng,Tang Chao-Shu,Zhang Jing. Taurine inhibits ischemia/reperfusion-induced compartment syndrome in rabbits[J]. Acta pharmacologica Sinica, 2005, 26(7): 821-827
Authors:Wang Ji-Xian  Li Yan  Zhang Li-Ke  Zhao Jing  Pang Yong-Zheng  Tang Chao-Shu  Zhang Jing
Affiliation:Institute of Cardiovascular Disease Research, The First Hospital of Peking University, Beijing 100034, China.
Abstract:Aim: To investigate effects of taurine on ischemia/reperfusion (I/R)-induced compartment syndrome in rabbit hind limbs. Methods: Rabbits underwent femoral artery occlusion after ligation of branches from terminal aorta to femoral artery. After a 7-h ischemia, reperfusion was established with the use of heparinized polyethylene shunts. Rabbits received taurine (1 g/kg) or normal saline (control) by iv infusion 10 min before shunt placement. During reperfusion, anterior compartment pressure (ACP) was monitored continuously in the left lower extremity. Gastrocnemius muscle triphenyltetrazolium chloride (TTC) level, taurine content and myeloperoxidase activity were assayed. Oxidative stress was induced in the in vitro gastrocnemius muscle slices by free radical generating systems (FRGS), and the malondialdehyde content was measured in presence or absence of taurine. Results: After 7 h of ischemia, none of the parameters that we measured were different from those before ischemia, except that TTC reduction decreased by 80%. In the control group, after 2 h of reperfusion, ACP increased 4.5-fold, and gastrocnemius muscle taurine content was reduced by 33%. In taurine-treated animals, at 2 h reperfusion, the mean arterial blood pressure and heart rate were increased, by 6% and 10%. ACP decreased by 39%, muscle edema decreased by 16%, TTC reduction increased by 150%, and lactate dehydrogenase decreased by 36% compared to control group. Plasma and muscle taurine content increased by 70% and 88%, respectively. In the taurine-treated group, at 2 h reperfusion, plasma malondialdehyde and conjugated diene content were decreased by 38% and 23%, respectively, and muscle malondialdehyde and conjugated diene content decreased by 22% and 30%, respectively compared to the control group. At 2 h reperfusion, myeloperoxidase activity was increased 3.5-fold in control animals. In the in vitro study, taurine decreased malondialdehyde content in muscle slices incubate dwith hypochlorous acid in a dose-dependent manner, but there was no change when incubated with hydrogen peroxide and xanthine oxidase. Conclusion: Treatment with taurine inhibited I/R-induced compartment syndrome by at least in part attenuating oxidative stress injury induced by I/R, suggesting clinical application of taurine might be a new strategy for the prevention and treatment of compartment syndrome.
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