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肠道微生物群在单端孢霉烯族霉菌毒素代谢中的作用。

The role of intestinal microflora in the metabolism of trichothecene mycotoxins.

作者信息

Swanson S P, Helaszek C, Buck W B, Rood H D, Haschek W M

机构信息

Department of Veterinary Biosciences, University of Illinois, Urbana 61801.

出版信息

Food Chem Toxicol. 1988 Oct;26(10):823-9. doi: 10.1016/0278-6915(88)90021-x.

DOI:10.1016/0278-6915(88)90021-x
PMID:3220324
Abstract

The role of faecal and intestinal microflora on the metabolism of trichothecene mycotoxins was examined in this study. Suspensions of microflora obtained from the faeces of horses, cattle, dogs, rats, swine and chickens were incubated anaerobically with the trichothecene mycotoxin, diacetoxyscirpenol (DAS). Micro-organisms from rats, cattle and swine completely biotransformed DAS, primarily to the deacylated deepoxidation products, deepoxy monoacetoxyscirpenol (DE MAS) and deepoxy scirpentriol (DE SCP). By contrast, faecal microflora from chickens, horses and dogs failed to reduce the epoxide group in DAS and yielded only the deacylation products, monoacetoxyscirpenol (MAS) and scirpentriol (SCP), in addition to unmetabolized parent compound. Intestinal microflora obtained from rats completely biotransformed DAS to DE MAS, DE SCP and SCP; and T-2 toxin to the deepoxy products, deepoxy HT-2 (DE HT-2) and deepoxy T-2 triol (DE TRIOL). Rat intestinal microflora also biotransformed the polar trichothecenes, T-2 tetraol and scirpentriol, to their corresponding deepoxy analogues. Deepoxy T-2 toxin (DE T-2) was synthesized from T-2 toxin and demonstrated to be 400 times less toxic than T-2 toxin in the rat skin irritation bioassay and non-toxic to mice given 60 mg/kg ip, demonstrating that epoxide reduction is a significant single step detoxification reaction for trichothecene mycotoxins.

摘要

本研究考察了粪便和肠道微生物群在单端孢霉烯族霉菌毒素代谢中的作用。将从马、牛、狗、大鼠、猪和鸡的粪便中获得的微生物群悬液与单端孢霉烯族霉菌毒素二乙酰氧基雪腐镰刀菌烯醇(DAS)进行厌氧培养。来自大鼠、牛和猪的微生物将DAS完全生物转化,主要转化为脱酰基的深度氧化产物,即深度氧化单乙酰氧基雪腐镰刀菌烯醇(DE MAS)和深度氧化蛇孢菌素醇(DE SCP)。相比之下,来自鸡、马和狗的粪便微生物群未能还原DAS中的环氧基团,除了未代谢的母体化合物外,仅产生脱酰基产物单乙酰氧基雪腐镰刀菌烯醇(MAS)和蛇孢菌素醇(SCP)。从大鼠获得的肠道微生物群将DAS完全生物转化为DE MAS、DE SCP和SCP;将T-2毒素转化为深度氧化产物,即深度氧化HT-2(DE HT-2)和深度氧化T-2三醇(DE TRIOL)。大鼠肠道微生物群还将极性单端孢霉烯族毒素T-2四醇和蛇孢菌素醇生物转化为其相应的深度氧化类似物。从T-2毒素合成了深度氧化T-2毒素(DE T-2),并在大鼠皮肤刺激生物测定中证明其毒性比T-2毒素低400倍,对腹腔注射60 mg/kg的小鼠无毒,这表明环氧化还原是单端孢霉烯族霉菌毒素的一个重要的单步解毒反应。

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