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培养的大鼠和人颊黏膜细胞对苯并[a]芘的代谢

Metabolism of benzo[a]pyrene by cultured rat and human buccal mucosa cells.

作者信息

Autrup H, Seremet T, Arenholt D, Dragsted L, Jepsen A

出版信息

Carcinogenesis. 1985 Dec;6(12):1761-5. doi: 10.1093/carcin/6.12.1761.

Abstract

Primary cultures of epithelial and fibroblast cells derived from human oral mucosa were studied for the ability to activate a tobacco smoke carcinogen, benzo[a]pyrene (BP). The cells were exposed to benzo[a]pyrene for 18 h. The cell-free medium was extracted with ethylacetate/acetone, and high-pressure liquid chromatography analysis of this fraction revealed that BP tetrols and diols were the major metabolites formed by both epithelial and fibroblast cells. However, the epithelial cells had a much higher rate of biotransformation of BP as measured by binding to cellular DNA. The mean binding level to human buccal mucosal DNA was among the highest observed in stratified human epithelia. The major BP-DNA adduct was formed by the reaction of the 'bay-region' BP diolepoxide with the exocyclic 2-amino group in guanine. In contrast to human cells, BP phenols and BP 9,10-diol were the major metabolites produced by primary epithelial and fibroblast cells derived from rat buccal mucosa. The DNA binding levels of BP in the two rat cell types were identical, and the binding level was several-fold lower than in the human epithelial cells. When an established rat tongue epithelial cell line (RTE 2) was treated with polycyclic aromatic hydrocarbons--BP and 7,12-dimethylbenz[a]-anthracene--a slight toxic effect was observed. Our results indicate that primary cultures of oral mucosa are able to metabolize BP into its ultimate carcinogenic form at a rate similar to or higher than other potential target tissues for BP-induced carcinogenesis.

摘要

对源自人口腔黏膜的上皮细胞和成纤维细胞的原代培养物进行了研究,以考察其激活烟草烟雾致癌物苯并[a]芘(BP)的能力。将细胞暴露于苯并[a]芘18小时。用乙酸乙酯/丙酮萃取无细胞培养基,对该馏分进行高压液相色谱分析,结果显示BP四醇和二醇是上皮细胞和成纤维细胞形成的主要代谢产物。然而,通过与细胞DNA结合来衡量,上皮细胞对BP的生物转化速率要高得多。与人颊黏膜DNA的平均结合水平是在分层人上皮中观察到的最高水平之一。主要的BP-DNA加合物是由“湾区”BP二环氧物与鸟嘌呤外环2-氨基反应形成的。与人类细胞不同,BP酚和BP 9,10-二醇是源自大鼠颊黏膜的原代上皮细胞和成纤维细胞产生的主要代谢产物。两种大鼠细胞类型中BP的DNA结合水平相同,且结合水平比人上皮细胞低几倍。当用多环芳烃——BP和7,12-二甲基苯并[a]蒽——处理已建立的大鼠舌上皮细胞系(RTE 2)时,观察到轻微的毒性作用。我们的结果表明,口腔黏膜原代培养物能够以与BP诱导致癌作用的其他潜在靶组织相似或更高的速率将BP代谢为其最终致癌形式。

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