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亚硝基苯在红细胞中对血红蛋白的氧化降解作用。

Oxidative degradation of haemoglobin by nitrosobenzene in the erythrocyte.

作者信息

Hirota K, Itano H A, Vedvick T S

出版信息

Biochem J. 1978 Sep 15;174(3):693-7. doi: 10.1042/bj1740693.

Abstract

Substitutions on the benzene ring of nitrosobenzene did not have the same effect on oxidative haemolysis as substitutions on phenylhydrazine. We previously found that the haemolytic effect of arylhydrazines paralleled their oxidative conversion into ligands of ferrihaemoglobin. In contrast, although most substituted nitrosobenzenes that are ligands of ferrohaemoglobin caused haemolysis and most that are not ligands failed to cause nitrosoarenes appeared to be related more closely to the ease of their reduction to arylhydroxylamines than to their properties as ligands. We propose a mechanism of oxidative degradation whereby the cyclic formation of phenylhydroxylamine from nitrosobenzene within an erythrocyte leads to the accumulation of H2O2, which then reacts with ferrohaemoglobin to initiate the oxidative cleavage of haem. The posulated active intermediate in this reaction is the same as that previously proposed in the oxidative degradation of haemoglobin by phenylhydrzine and in the coupled oxidation of ascorbic acid and haemoglobin.

摘要

亚硝基苯苯环上的取代基对氧化溶血的影响与苯肼上的取代基不同。我们之前发现芳基肼的溶血作用与其氧化转化为高铁血红蛋白配体的过程平行。相比之下,虽然大多数作为亚铁血红蛋白配体的取代亚硝基苯会引起溶血,而大多数不是配体的则不会,但亚硝基芳烃似乎与其还原为芳基羟胺的难易程度关系更为密切,而非与其作为配体的性质有关。我们提出了一种氧化降解机制,即红细胞内亚硝基苯环化形成苯羟胺会导致过氧化氢积累,然后过氧化氢与亚铁血红蛋白反应引发血红素的氧化裂解。该反应中假定的活性中间体与之前在苯肼氧化降解血红蛋白以及抗坏血酸和血红蛋白偶联氧化中提出的中间体相同。

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本文引用的文献

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The intracellular and membrane effects of oxidant agents on normal red cells.
Br J Haematol. 1970 Sep;19(3):417-28. doi: 10.1111/j.1365-2141.1970.tb01638.x.

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