Effect of Dexrazoxane on Homocysteine-Induced Endothelial Dysfunction in Normal Subjects

Haoyi Zheng, C. Dimayuga, Alhakam Hudaihed, S. Katz
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引用次数: 30

Abstract

Objective—Dexrazoxane is an antioxidant prodrug that on hydrolysis is converted into an intracellular iron chelator. We hypothesized that the antioxidant effects of dexrazoxane would prevent homocysteine-induced endothelial dysfunction in the brachial artery of normal human subjects. Methods and Results—Ten healthy volunteers completed a randomized, double-blind, crossover study. Plasma homocysteine levels and brachial artery endothelium-dependent (flow-mediated dilation [FMD]) and endothelium-independent (sublingual nitroglycerin) responses were measured before and 4 hours after ingestion of l-methionine (100 mg/kg), preceded by intravenous administration of dexrazoxane (500 mg/m2) or placebo over 30 minutes. After placebo, oral methionine increased plasma homocysteine (from 5.1±0.4 &mgr;mol/L at baseline to 14.2±1.3 &mgr;mol/L at 4 hours, P <0.001) and decreased FMD (from 3.8±0.7% at baseline to 1.2±0.5% at 4 hours, P =0.02). Dexrazoxane did not change homocysteine concentrations after methionine administration (14.9±1.1 &mgr;mol/L at 4 hours, P =0.29 versus placebo) but did completely abrogate the homocysteine-induced reduction in FMD (from 3.5±0.5% at baseline to 5.9±1.1% at 4 hours, P <0.01 versus placebo). Endothelium-independent responses to sublingual nitroglycerin did not differ after the administration of placebo and dexrazoxane. Conclusions—Administration of the novel antioxidant agent dexrazoxane prevents homocysteine-induced impairment of vascular endothelial function in the brachial artery of healthy subjects.
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右拉唑烷对正常人同型半胱氨酸诱导的内皮功能障碍的影响
目的:dexrazoxane是一种抗氧化前药,水解后可转化为细胞内铁螯合剂。我们假设dexrazoxane的抗氧化作用可以预防正常人同型半胱氨酸诱导的肱动脉内皮功能障碍。方法与结果:10名健康志愿者完成了一项随机、双盲、交叉研究。血浆同型半胱氨酸水平和肱动脉内皮依赖性(血流介导扩张[FMD])和内皮非依赖性(舌下硝酸甘油)反应在摄入l-蛋氨酸(100 mg/kg)前和4小时后测量,然后静脉给药dexrazoxane (500 mg/m2)或安慰剂超过30分钟。服用安慰剂后,口服蛋氨酸增加血浆同型半胱氨酸(从基线时的5.1±0.4 mol/L增加到4小时时的14.2±1.3 mol/L, P <0.001)并降低FMD(从基线时的3.8±0.7%减少到4小时时的1.2±0.5%,P =0.02)。右拉唑环在给药蛋氨酸后没有改变同型半胱氨酸浓度(4小时时为14.9±1.1 mol/L,与安慰剂相比P =0.29),但完全消除了同型半胱氨酸诱导的FMD降低(从基线时的3.5±0.5%降至4小时时的5.9±1.1%,与安慰剂相比P <0.01)。在给予安慰剂和右拉唑环后,舌下硝酸甘油的内皮非依赖性反应没有差异。结论:新型抗氧化剂右拉唑烷可预防同型半胱氨酸引起的肱动脉血管内皮功能损伤。
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