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抗疟药伯氨喹在小鼠肝脏酶作用下的体外代谢及一种形成高铁血红蛋白代谢物的鉴定。

In vitro metabolism of the antimalarial agent primaquine by mouse liver enzymes and identification of a methemoglobin-forming metabolite.

作者信息

Strother A, Allahyari R, Buchholz J, Fraser I M, Tilton B E

出版信息

Drug Metab Dispos. 1984 Jan-Feb;12(1):35-44.

PMID:6141909
Abstract

From a mouse liver microsomal system, we have isolated and identified a methemoglobin-forming metabolite of primaquine (PQ). Evidence has been found for both O-dealkylation and hydroxylation of PQ to form a metabolite, 5,6-dihydroxy-8-(4-amino-1-methylbutylamino)quinoline, which is highly active in forming methemoglobin in both normal and glucose-6-phosphate dehydrogenase-deficient erythrocytes. It also actively decreases glutathione levels in glucose-6-phosphate dehydrogenase-deficient erythrocytes. The inhibitor SKF 525-A prevented metabolite formation while iproniazid and carbon monoxide did not inhibit metabolism completely but may have resulted in formation of a different unidentified metabolite. Mass spectrometry, HPLC, NMR, and other more indirect methods were used to help identify the metabolite. It was identified indirectly via a blue compound which results from extracting the actual metabolite from the incubation mixture with organic solvents under alkaline conditions in the presence of light. The blue compound was identified as a quinonimine in which the 8-amino side chain of PQ cyclizes to produce a third ring system.

摘要

我们从小鼠肝脏微粒体系统中分离并鉴定出了伯氨喹(PQ)的一种可形成高铁血红蛋白的代谢产物。已发现PQ经O-脱烷基化和羟基化形成一种代谢产物,即5,6-二羟基-8-(4-氨基-1-甲基丁基氨基)喹啉,该产物在正常和葡萄糖-6-磷酸脱氢酶缺乏的红细胞中形成高铁血红蛋白的活性都很高。它还能使葡萄糖-6-磷酸脱氢酶缺乏的红细胞中的谷胱甘肽水平显著降低。抑制剂SKF 525-A可阻止代谢产物的形成,而异烟肼和一氧化碳虽不能完全抑制代谢,但可能导致形成了一种不同的未鉴定代谢产物。使用质谱、高效液相色谱、核磁共振及其他更间接的方法来辅助鉴定该代谢产物。它是通过一种蓝色化合物间接鉴定出来的,该蓝色化合物是在碱性条件下、有光存在时,用有机溶剂从孵育混合物中提取实际代谢产物而得到的。该蓝色化合物被鉴定为一种醌亚胺,其中PQ的8-氨基侧链环化形成了第三个环系统。

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