小鼠和猴的肝脏匀浆在体外将T-2毒素转化为3'-羟基T-2毒素和3'-羟基HT-2毒素。
In vitro formation of 3'-hydroxy T-2 and 3'-hydroxy HT-2 toxins from T-2 toxin by liver homogenates from mice and monkeys.
作者信息
Yoshizawa T, Sakamoto T, Okamoto K
出版信息
Appl Environ Microbiol. 1984 Jan;47(1):130-4. doi: 10.1128/aem.47.1.130-134.1984.
Abstract
In vitro metabolism of T-2 toxin was studied in homogenates of mouse and monkey livers. In addition to several hydrolyzed products, including HT-2 toxin, neosolaniol, 4-deacetylneosolaniol, 15-deacetylneosolaniol, and T-2 tetraol, two metabolic products were isolated from the incubation mixture. Their structures were confirmed as 3'-hydroxy T-2 toxin and 3'-hydroxy HT-2 toxin on the basis of mass and nuclear magnetic resonance spectroscopy. The formation of these hydroxylated metabolites was found in the microsomes in the presence of NADPH, and the hydroxylation reaction was enhanced by treating mice with phenobarbital. The results suggest that a cytochrome P-450 is catalyzing the hydroxylation at the C-3' position of T-2 and HT-2 toxins. An in vitro metabolic pathway of T-2 toxin in the hepatic homogenates containing the NADPH-generating system is proposed.
摘要
在小鼠和猴肝脏匀浆中研究了T-2毒素的体外代谢。除了几种水解产物,包括HT-2毒素、新茄病镰刀菌烯醇、4-脱乙酰基新茄病镰刀菌烯醇、15-脱乙酰基新茄病镰刀菌烯醇和T-2四醇外,还从孵育混合物中分离出两种代谢产物。根据质谱和核磁共振光谱,确定它们的结构为3'-羟基T-2毒素和3'-羟基HT-2毒素。在微粒体中,存在NADPH时可发现这些羟基化代谢产物的形成,用苯巴比妥处理小鼠可增强羟基化反应。结果表明,细胞色素P-450催化T-2和HT-2毒素C-3'位的羟基化反应。提出了含NADPH生成系统的肝脏匀浆中T-2毒素的体外代谢途径。
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