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六氯苯及其代谢产物在原代肝细胞培养中的生物转化和致卟啉作用。

Biotransformation and porphyringogenic action of hexachlorobenzene and its metabolites in a primary liver cell culture.

作者信息

Debets F M, Reinders J H, Debets A J, Lössbroek T G, Strik J J, Koss G

出版信息

Toxicology. 1981;19(3):185-96. doi: 10.1016/0300-483x(81)90128-1.

Abstract

Hexachlorobenzene (HCB) is metabolized in a primary culture of chick embryo liver cells and causes porphyrin accumulation within 24 h after administration. The HCB-metabolites, pentachlorothiophenol (PCThP), pentachlorobenzene (PeCB) and pentachlorophenol (PCP) identified in liver cell culture are already known from long-term experiments with rats. The pattern of accumulated porphyrins is comparable with the pathological porphyrin pattern observed in oral feeding studies with warm blooded laboratory animals. Protein bound radioactivity was found in cell cultures treated with [14C] HCB. Addition of the monooxygenase-inhibitor piperonyl butoxide or ascorbic acid decreased the irreversible binding of 14C-metabolites. The results show that biotransformation of HCB fulfils an essential role in the onset of porphyria. Since none of the main HCB-metabolites could induce a pathological porphyrin pattern, a reactive intermediate capable of reacting with glutathione or thiol-groups of uroporphyrinogen decarboxylase (UROG-D) is believed to be responsible for the inhibition of UROG-D. The chick embryo liver cell system may be considered as a useful and sensitive system for studying the metabolism of xenobiotics in relation to their toxicity.

摘要

六氯苯(HCB)在鸡胚肝细胞原代培养物中发生代谢,并在给药后24小时内导致卟啉积累。在肝细胞培养物中鉴定出的HCB代谢物,五氯硫酚(PCThP)、五氯苯(PeCB)和五氯酚(PCP),在对大鼠的长期实验中就已为人所知。积累的卟啉模式与在温血实验动物口服喂养研究中观察到的病理性卟啉模式相当。在用[14C]HCB处理的细胞培养物中发现了蛋白质结合放射性。添加单加氧酶抑制剂胡椒基丁醚或抗坏血酸可降低14C代谢物的不可逆结合。结果表明,HCB的生物转化在卟啉病的发病过程中起重要作用。由于HCB的主要代谢物均不能诱导病理性卟啉模式,因此认为一种能够与尿卟啉原脱羧酶(UROG-D)的谷胱甘肽或硫醇基团反应的活性中间体是抑制UROG-D的原因。鸡胚肝细胞系统可被视为研究外源化合物代谢与其毒性关系的有用且敏感的系统。

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