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Celecoxib enhances the detoxification of diethylnitrosamine in rat liver cancer

机译:塞来昔布增强大鼠肝癌中二乙基亚硝胺的解毒作用

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摘要

AIM: To study the effect of celecoxib (CXB) on diethylnitrosamine activation through the regulation of cytochrome P450 in a hepatocarcinogenesis model.METHODS: Six-week-old male Sprague-Dawley rats were randomly divided into five groups, a non-treated group (NT), a diethylnitrosamine-treated group (DEN), a DEN+CXB-treated group (DEN+CXB), and CXB 8 d-treated and CXB 32 d-treated groups. The effects of celecoxib on the enzymatic activities of CYP1A1, 2A, 2B1/2, and 2E1 were assessed in hepatic microsomes 24 h after DEN administration. Changes in CYP1A1 and CYP2B1/2 protein expression were also evaluated. The rate of DEN metabolism was measured by the production of the deethylation metabolite acetaldehyde, and the denitrosation metabolite nitrite.RESULTS: DEN+CXB administration produced a significant increase in the enzymatic activities of CYP2B1/2 and 1A1, whereas it did not change the activities of CYP2A and 2E1, compared to that of the DEN group. CXB treatment for eight days did not produce a significant effect on enzymatic activity when compared to the NT group; however, when it was administered for prolonged times (CXB 32 d group), the enzymatic activities were increased in a similar pattern to those in the DEN+CXB group. The observed increase in the enzymatic activities in the DEN+CXB group was accompanied by an increase in the CYP2B1/2 protein levels; no changes were observed in the levels of CYP1A1. In vitro, CXB increased the denitrosation of DEN, a pathway of metabolic detoxification. The addition of SKF-525A, a preferential inhibitor of CYP2B, abrogated the denitrosation of DEN.CONCLUSION: These results suggest that the mechanism of action of CXB involves enhancement of the detoxification of DEN by an increasing denitrosation via CYP2B1/2.
机译:目的:研究在肝癌发生模型中塞来昔布(CXB)通过调节细胞色素P450对二乙基亚硝胺活化的作用。方法:将六周大的雄性Sprague-Dawley大鼠随机分为五组,未治疗组( NT),二乙基亚硝胺处理组(DEN),DEN + CXB处理组(DEN + CXB)以及CXB 8 d处理和CXB 32 d处理的组。 DEN给药后24小时,在肝微粒体中评价了celecoxib对CYP1A1、2A,2B1 / 2和2E1酶活性的影响。还评估了CYP1A1和CYP2B1 / 2蛋白表达的变化。 DEN的代谢速率通过脱乙基代谢产物乙醛和脱硝代谢产物亚硝酸盐的产生来衡量。结果:DEN + CXB给药使CYP2B1 / 2和1A1的酶活性显着增加,而没有改变CYP2B1 / 2和1A1的酶活性。 CYP2A和2E1与DEN组比较。与NT组相比,连续八天的CXB处理对酶活性没有显着影响。但是,长时间服用(CXB 32 d组)时,酶活性以与DEN + CXB组相似的方式增加。在DEN + CXB组中观察到的酶活性增加伴随着CYP2B1 / 2蛋白水平的增加; CYP1A1水平未见变化。在体外,CXB增加了DEN的脱硝作用,DEN是一种代谢排毒的途径。结论CYP2B的优先抑制剂SKF-525A消除了DEN的脱硝作用。结论:这些结果表明CXB的作用机制包括通过CYP2B1 / 2的增加的脱氮作用来增强DEN的脱毒作用。

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