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关于黄曲霉毒素B1对大鼠肝细胞的细胞毒性与该毒素代谢之间关系的一些研究。

Some studies on the relationship between the cytotoxicity of aflatoxin B1 to rat hepatocytes and metabolism of the toxin.

作者信息

Metcalfe S A, Neal G E

出版信息

Carcinogenesis. 1983 Aug;4(8):1013-9. doi: 10.1093/carcin/4.8.1013.

Abstract

Aflatoxin B1 (AFB1) caused marked, rapid (1 h) inhibition of RNA synthesis and subsequent cytotoxic response in isolated and primary cultured hepatocytes, from control rats, which are known to metabolise AFB1. A rat liver-derived cell line, BL8L, was much less susceptible to these effects of AFB1. These cells have no detectable AFB1 metabolising capacity, but a less potent, anti-mitotic action of AFB1 was observed in the BL8L cell line. Thus AFB1 would seem to require metabolism to exert its acute cytotoxic action which is found at very low AFB1 concentrations, although a direct antimitotic effect, independent of metabolism, is seen in dividing cells. Phenobarbitone and 3-methylcholanthrene in vivo pretreatments, known inducers of AFB1 metabolism, resulted in reduced AFB1 inhibition of RNA synthesis and cytotoxicity in hepatocytes, but only at lower concentrations of AFB1 used, whereas cells from AFB1 fed rats were much less susceptible to AFB1 toxicity at all concentrations used. This resistance to cytotoxicity of AFB1 would appear to involve detoxification mechanisms, primarily the formation of polar conjugates of AFB1 metabolites, particularly glutathione conjugates. These cell culture systems are useful for studying association between metabolism and cytotoxicity of AFB1, and other xenobiotics.

摘要

黄曲霉毒素B1(AFB1)在来自对照大鼠的分离的原代培养肝细胞中,引发了显著且迅速(1小时)的RNA合成抑制以及随后的细胞毒性反应,已知这些肝细胞能够代谢AFB1。一种源自大鼠肝脏的细胞系BL8L对AFB1的这些作用的敏感性要低得多。这些细胞没有可检测到的AFB1代谢能力,但在BL8L细胞系中观察到AFB1具有较弱的抗有丝分裂作用。因此,AFB1似乎需要代谢才能发挥其急性细胞毒性作用,这种作用在非常低的AFB1浓度下即可发现,尽管在分裂细胞中可以看到与代谢无关的直接抗有丝分裂作用。体内预先用苯巴比妥和3 - 甲基胆蒽处理,这两种已知的AFB1代谢诱导剂,导致AFB1对肝细胞RNA合成的抑制和细胞毒性降低,但仅在使用较低浓度的AFB1时才出现这种情况,而来自喂食AFB1大鼠的细胞在所有使用的浓度下对AFB1毒性的敏感性都要低得多。对AFB1细胞毒性的这种抗性似乎涉及解毒机制,主要是AFB1代谢物形成极性共轭物,特别是谷胱甘肽共轭物。这些细胞培养系统对于研究AFB1以及其他外源化合物的代谢与细胞毒性之间的关联很有用。

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