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在存在烟酰胺腺嘌呤二核苷酸磷酸(NADPH)或烟酰胺腺嘌呤二核苷酸(NADH)的情况下,人肝微粒体产生活性氧中间体。

Generation of reactive oxygen intermediates by human liver microsomes in the presence of NADPH or NADH.

作者信息

Rashba-Step J, Cederbaum A I

机构信息

Department of Biochemistry, Mount Sinai School of Medicine, New York, NY 10029.

出版信息

Mol Pharmacol. 1994 Jan;45(1):150-7.

PMID:8302274
Abstract

Studies were carried out to evaluate the ability of human liver microsomes to generate superoxide radical and hydrogen peroxide, and to interact with ferric chelates to produce more potent oxidizing species such as the hydroxyl radical (.OH). In the presence of either NADPH or NADH, human liver microsomes produced superoxide and H2O2 at rates about 20 to 30% of that found with rat liver microsomes. These lower rates are caused, in part, by the 3-fold lower content of total cytochrome P450 in the human liver microsomes. NADH-dependent rates were about 25 to 30% of the NADPH-dependent rates. In the presence of appropriate ferric complexes, human liver microsomes generated .OH, promoted cleavage of vicinal diols, and underwent lipid peroxidation. In contrast to results with rat liver microsomes, NADH-dependent rates of .OH production or lipid peroxidation by human liver microsomes were similar to the NADPH-dependent rates. Human liver microsomes reduced ferric ATP or ferric EDTA at nearly comparable rates with NADPH and NADH. Sensitivity of the various iron-dependent reactions to antioxidants was found to be characteristic of the particular system. These results suggest the possibility that human liver microsomes are an important source of reactive oxygen intermediates, especially under conditions of increased NADH or NADPH availability and elevated iron concentration.

摘要

开展了多项研究,以评估人肝微粒体产生超氧阴离子自由基和过氧化氢的能力,以及与铁螯合物相互作用以产生更具活性的氧化物种(如羟基自由基·OH)的能力。在存在NADPH或NADH的情况下,人肝微粒体产生超氧阴离子和H2O2的速率约为大鼠肝微粒体的20%至30%。这些较低的速率部分是由于人肝微粒体中细胞色素P450的总含量低3倍所致。依赖NADH的速率约为依赖NADPH速率的25%至30%。在存在适当的铁络合物时,人肝微粒体产生·OH,促进邻二醇的裂解,并发生脂质过氧化。与大鼠肝微粒体的结果相反,人肝微粒体依赖NADH产生·OH或脂质过氧化的速率与依赖NADPH的速率相似。人肝微粒体以与NADPH和NADH几乎相当的速率还原铁ATP或铁EDTA。发现各种铁依赖性反应对抗氧化剂的敏感性是特定系统的特征。这些结果表明,人肝微粒体有可能是活性氧中间体的重要来源,尤其是在NADH或NADPH可用性增加以及铁浓度升高的情况下。

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