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Spontaneous Production of Glutathione-Conjugated Forms of 12-Dichloropropane: Comparative Study on Metabolic Activation Processes of Dihaloalkanes Associated with Occupational Cholangiocarcinoma

机译:谷胱甘肽共轭形式的12-二氯丙烷的自发生产:与职业性胆管癌相关的二卤代烷烃代谢活化过程的比较研究

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摘要

Recently, epidemiological studies revealed a positive relationship between an outbreak of occupational cholangiocarcinoma and exposure to organic solvents containing 1,2-dichloropropane (1,2-DCP). In 1,2-DCP-administered animal models, we previously found biliary excretion of potentially oncogenic metabolites consisting of glutathione- (GSH-) conjugated forms of 1,2-DCP (GS-DCPs); however, the GS-DCP production pathway remains unknown. To enhance the understanding of 1,2-DCP-related risks to human health, we examined the reactivity of GSH with 1,2-DCP in vitro and compared it to that with dichloromethane (DCM), the other putative substance responsible for occupational cholangiocarcinoma. Our results showed that 1,2-DCP was spontaneously conjugated with GSH, whereas this spontaneous reaction was hardly detected between DCM and GSH. Further analysis revealed that glutathione S-transferase theta 1 (GSTT1) exhibited less effect on the 1,2-DCP reaction as compared with that observed for DCM. Although GSTT1-mediated bioactivation of dihaloalkanes could be a plausible explanation for the production of reactive metabolites related to carcinogenesis based on previous studies, this catalytic pathway might not mainly contribute to 1,2-DCP-related occupational cholangiocarcinoma. Considering the higher catalytic activity of GSTT1 on DCM as compared with that on 1,2-DCP, our findings suggested differences in the activation processes associated with 1,2-DCP and DCM metabolism.
机译:最近,流行病学研究显示职业性胆管癌的爆发与接触含有1,2-二氯丙烷(1,2-DCP)的有机溶剂之间存在正相关关系。在1,2-DCP施用的动物模型中,我们先前发现了由谷胱甘肽-(GSH-)共轭形式的1,2-DCP(GS-DCPs)组成的潜在致癌代谢产物的胆汁排泄;但是,GS-DCP的生产途径仍然未知。为了加深对1,2-DCP相关的人类健康风险的了解,我们在体外检查了GSH与1,2-DCP的反应性,并将其与负责职业性胆管癌的另一种假定物质二氯甲烷(DCM)进行了比较。 。我们的结果表明,1,2-DCP与GSH自发偶联,而在DCM和GSH之间几乎没有检测到这种自发反应。进一步的分析表明,与DCM相比,谷胱甘肽S-转移酶theta 1(GSTT1)对1,2-DCP反应的影响较小。尽管根据先前的研究,GSTT1介导的二卤代烷烃的生物活化可能是与致癌作用有关的反应性代谢产物产生的合理解释,但该催化途径可能主要不是导致1,2-DCP相关的职业性胆管癌。考虑到GSTT1对DCM的催化活性高于1,2-DCP的催化活性,我们的发现表明与1,2-DCP和DCM代谢相关的活化过程存在差异。

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