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大鼠体内黄曲霉毒素B1的代谢:多卤代联苯增强其向黄曲霉毒素M1的转化。

Aflatoxin B1 metabolism in the rat: polyhalogenated biphenyl enhanced conversion to aflatoxin M1.

作者信息

Shepherd E C, Phillips T D, Irvin T R, Safe S H, Robertson L W

出版信息

Xenobiotica. 1984 Sep;14(9):741-50. doi: 10.3109/00498258409151472.

Abstract

The effects of polychlorinated biphenyls (PCBs) and polybrominated biphenyls (PBBs) on the formation in vitro of aflatoxin Q1 and aflatoxin M1 from aflatoxin B1 by rat-liver microsomes were investigated. AFB1 metabolism by hepatic microsomes from PBB- and PCB-treated rats resulted in 16- and 30-fold increases, respectively, in levels of aflatoxin M1. The enhanced formation of aflatoxin M1 did not correlate with PBB and PCB stimulation of benzo[a]pyrene hydroxylase (AHH) activity. Studies in vivo clearly demonstrated enhanced secretion of aflatoxin M1 by female lactating rats with prior exposure to PCBs. PCB pretreatment enhanced the activity of mammary as well as hepatic tissue microsomal preparations in converting aflatoxin B1 to aflatoxin M1. Our findings indicate that PCB exposure increases the production of aflatoxin M1 in vitro and also increases the levels of aflatoxin M1 released into the milk.

摘要

研究了多氯联苯(PCBs)和多溴联苯(PBBs)对大鼠肝脏微粒体将黄曲霉毒素B1体外转化为黄曲霉毒素Q1和黄曲霉毒素M1的影响。用PBBs和PCBs处理过的大鼠肝脏微粒体对AFB1的代谢作用,分别使黄曲霉毒素M1的水平提高了16倍和30倍。黄曲霉毒素M1生成的增加与PBBs和PCBs对苯并[a]芘羟化酶(AHH)活性的刺激作用无关。体内研究清楚地表明,预先接触PCBs的雌性泌乳大鼠黄曲霉毒素M1的分泌增加。PCB预处理增强了乳腺以及肝脏组织微粒体制剂将黄曲霉毒素B1转化为黄曲霉毒素M1的活性。我们的研究结果表明,接触PCB会增加体外黄曲霉毒素M1的产生,也会增加释放到乳汁中的黄曲霉毒素M1的水平。

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