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首页> 外文期刊>Chemico-biological interactions >Lack of contribution of covalent benzo(a)pyrene-7,8-quinone-DNA adducts in benzo(a)pyrene-induced mouse lung tumorigenesis.
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Lack of contribution of covalent benzo(a)pyrene-7,8-quinone-DNA adducts in benzo(a)pyrene-induced mouse lung tumorigenesis.

机译:在苯并(a)-诱导的小鼠肺肿瘤发生中缺乏共价苯并(a)-7-7,8-醌-DNA加合物的贡献。

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Benzo[a]pyrene (B[a]P) is a potent human and rodent lung carcinogen. This activity has been ascribed in part to the formation of anti-trans-7,8-dihydroxy-7,8-dihydroB[a]P-9,10-epoxide (BPDE)-DNA adducts. Other carcinogenic mechanisms have been proposed: (1) the induction of apurinic sites from radical cation processes, and (2) the metabolic formation of B[a]P-7,8-quinone (BPQ) that can form covalent DNA adducts or reactive oxygen species which can damage DNA. The studies presented here sought to examine the role of stable BPQ-DNA adducts in B[a]P-induced mouse lung tumorigenesis. Male strain A/J mice were injected intraperitoneally once with BPQ or trans-7,8-dihydroxy-7,8-dihydroB[a]P (BP-7,8-diol) at 30, 10, 3, or 0mg/kg. Lungs and livers were harvested after 24h, the DNA extracted and subjected to (32)P-postlabeling analysis. Additional groups of mice were dosed once with BPQ or BP-7,8-diol each at 30 mg/kg and tissues harvested 48 and 72 h later, or with B[a]P (50mg/kg, a tumorigenic dose) and tissues harvested 72 h later. No BPQ or any other DNA adducts were observed in lung or liver tissues 24, 48, or 72 h after the treatment with 30 mg/kg BPQ. BP-7,8-diol gave BPDE-DNA adducts at all time points in both tissues and B[a]P treatment gave BPDE-DNA adducts in the lung. In each case, no BPQ-DNA adducts were detected. Mouse body weights significantly decreased over time after BPQ or BP-7,8-diol treatments suggesting that systemic toxicity was induced by both agents. Model studies with BPQ and N-acetylcysteine suggested that BPQ is rapidly inactivated by sulfhydryl-containing compounds and not available for DNA adduction. We conclude that under these treatment conditions BPQ does not form stable covalent DNA adducts in the lungs or livers of strain A/J mice, suggesting that stable BPQ-covalent adducts are not a part of the complex of mechanisms involved in B[a]P-induced mouse lung tumorigenesis.
机译:苯并[a] py(B [a] P)是一种强力的人类啮齿动物肺致癌物。此活性部分归因于抗反式7,8-二羟基-7,8-二氢B [a] P-9,10-环氧(BPDE)-DNA加合物的形成。还提出了其他致癌机理:(1)从自由基阳离子过程诱导嘌呤位点,(2)可以形成共价DNA加合物或反应性的B [a] P-7,8-醌(BPQ)的代谢形成会破坏DNA的氧。此处提出的研究试图检查稳定的BPQ-DNA加合物在B [a] P诱导的小鼠肺肿瘤发生中的作用。以30、10、3或0mg / kg的剂量向BPQ或trans-7,8-dihydroxy-7,8-dihydroB [a] P(BP-7,8-diol)腹膜内注射一次雄性A / J小鼠。 24小时后收获肺和肝脏,提取DNA并进行(32)P-后标记分析。其他组的小鼠分别以30 mg / kg的剂量分别服用BPQ或BP-7,8-二醇,并在48和72小时后收获组织,或以B [a] P(50mg / kg,致瘤剂量)和组织给药72小时后收获。用30 mg / kg BPQ治疗后24、48或72 h在肺或肝组织中未观察到BPQ或任何其他DNA加合物。 BP-7,8-二醇在两个组织的所有时间点均产生BPDE-DNA加合物,而B [a] P处理则在肺部产生BPDE-DNA加合物。在每种情况下,均未检测到BPQ-DNA加合物。 BPQ或BP-7,8-二醇处理后,小鼠体重随时间显着下降,表明这两种药物均可引起全身毒性。用BPQ和N-乙酰基半胱氨酸进行的模型研究表明,BPQ被含巯基的化合物迅速失活,不能用于DNA加成。我们得出的结论是,在这些治疗条件下,BPQ在品系A / J小鼠的肺或肝中不会形成稳定的共价DNA加合物,这表明稳定的BPQ-共价加合物不是B [a] P参与的机制复杂的一部分诱导的小鼠肺肿瘤发生。

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