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辐射防护剂对肝脏微粒体羟化系统的生化作用:体外研究

Biochemical effects on radioprotective agents on the liver microsomal hydroxylating system: in vitro studies.

作者信息

Bonfils C, Debey P, Balny C

出版信息

Int J Radiat Biol Relat Stud Phys Chem Med. 1978 Jun;33(6):531-40. doi: 10.1080/09553007814550441.

Abstract

The action of two radioprotectors--cysteamine and cystamine--on the liver microsomal multi-enzyme hydroxylating system, a key stem in drug and biological compounds metabolism, has been studied. Their effects have been systematically analysed at the level of individual enzyme activities and global functions. The two compounds are quite inactive on NADPH and NADH cytochrome c reductase activities, but slightly denature the cytochrome P450 into cytochrome P420. Furthermore, they do inhibit to some extent (30 per cent at 10(-2) M) the rate of codeine hydroxylation and totally suppress ((at 10(-2) M) the NADPH-induced lipid peroxidation which occurs during enzymatic functioning. These results are discussed in the light of the toxicity of radioprotectors.

摘要

已对两种辐射防护剂——半胱胺和胱胺——对肝脏微粒体多酶羟化系统(药物和生物化合物代谢的关键环节)的作用进行了研究。已在个体酶活性和整体功能水平上对它们的作用进行了系统分析。这两种化合物对NADPH和NADH细胞色素c还原酶活性相当无活性,但会使细胞色素P450轻微变性为细胞色素P420。此外,它们在一定程度上(10⁻² M时为30%)抑制可待因羟化速率,并完全抑制(10⁻² M时)酶促功能过程中发生的NADPH诱导的脂质过氧化。根据辐射防护剂的毒性对这些结果进行了讨论。

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