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硝呋替莫和苯硝唑在大鼠乳腺组织细胞成分中的代谢。

Metabolization of nifurtimox and benznidazole in cellular fractions of rat mammary tissue.

机构信息

Centro de Investigaciones Toxicológicas (CEITOX-CITEFA/ CONICET), Buenos Aires, Argentina.

出版信息

Hum Exp Toxicol. 2010 Oct;29(10):813-22. doi: 10.1177/0960327110361756. Epub 2010 Feb 11.

Abstract

Two nitroheterocyclic drugs, nifurtimox (NFX) and benznidazole (BZ), used in the treatment of Chagas' disease have serious side effects attributed to their nitroreduction to reactive metabolites. Here, we report that these drugs reach the mammary tissue and there they could undergo in situ bioactivation. Both were detected in mammary tissue from female Sprague-Dawley rats after their intragastric administration. Only NFX was biotransformed by pure xanthine-oxidoreductase and from tissue cytosol. These activities were purine dependent and were inhibited by allopurinol. Also, only NFX was biotransformed by microsomes in the presence of β-nicotinamide adenine dinucleotide phosphate, reduced form (NADPH), and was inhibited by carbon monoxide and partially by diphenyleneiodonium. NFX treatment produced significant decrease in protein sulfhydryl content after 1, 3 and 6 hours; no increases in protein carbonyl content at any time tested and significantly higher levels of lipid hydroperoxides at 3 and 6 hours; besides, ultrastructural observations after 24 hours showed significant differences in epithelial cells compared to control. These findings indicate that NFX might be more deleterious to mammary tissue than BZ and could correlate with early reports on its ability to promote rat mammary tissue toxicity.

摘要

两种硝基杂环药物,硝呋替莫(NFX)和苯并硝唑(BZ),用于治疗恰加斯病,但具有严重的副作用,归因于它们的硝基还原为反应性代谢物。在这里,我们报告这些药物到达乳腺组织,在那里它们可以进行原位生物激活。在雌性 Sprague-Dawley 大鼠口服给药后,两种药物都在乳腺组织中被检测到。只有 NFX 被纯黄嘌呤氧化还原酶和组织胞浆转化。这些活性依赖于嘌呤,并被别嘌呤醇抑制。此外,只有 NFX 在存在 β-烟酰胺腺嘌呤二核苷酸磷酸(还原型)、一氧化碳和二苯乙烯碘的情况下被微粒体转化,并被部分抑制。NFX 处理后 1、3 和 6 小时,蛋白质巯基含量显著下降;在任何测试时间均未增加蛋白质羰基含量,在 3 和 6 小时时脂质过氧化物水平显著升高;此外,24 小时的超微结构观察显示,与对照组相比,上皮细胞有明显差异。这些发现表明,NFX 可能对乳腺组织比 BZ 更具危害性,这与早期关于其促进大鼠乳腺组织毒性的报道相吻合。

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