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Fpg和Endo III在人淋巴细胞和L5178Y小鼠淋巴瘤细胞长期培养中对儿茶酚诱导的DNA损伤的不同作用。

Different roles of Fpg and Endo III on catechol-induced DNA damage in extended-term cultures of human lymphocytes and L5178Y mouse lymphoma cells.

作者信息

Andersson Maria A, Hellman Björn E

机构信息

Department of Pharmaceutical Biosciences, Division of Toxicology, Box 594, BMC, SE-751 24 Uppsala, Sweden.

出版信息

Toxicol In Vitro. 2005 Sep;19(6):779-86. doi: 10.1016/j.tiv.2005.04.011.

Abstract

Catechol is a genotoxic agent assumed to induce DNA damage via the oxidative pathway. Using the comet assay and the repair-specific enzymes formamido pyrimidine glycosylase (Fpg) and endonuclease III (Endo III), we examined the ability of catechol to induce DNA damage in extended-term cultures of human lymphocytes and mouse lymphoma cells. Our results suggest that mouse lymphoma cells are somewhat more sensitive towards catechol-induced DNA damage than the extended-term cultures of human lymphocytes. At high concentrations, the catechol-induced damage seemed to be independent of both Fpg and Endo III, possibly indicating a non-oxidative pathway for the DNA damage (involving, for example, a bulky adduct). The fact that Endo III, but not Fpg, enhanced the DNA damaging effect of catechol, suggests that this metabolite of benzene either mediates oxidation of pyrimidines rather than purines, or that oxidised purines are repaired more efficiently, at least in human lymphocytes. In the latter cells, low concentrations of catechol were found to reduce the DNA migration. Considering the role of Fpg and it's adduct specific detection of 8-oxoguanine, this suggests that a low concentration of catechol has an antioxidative effect reducing the background levels of oxidized purines.

摘要

儿茶酚是一种遗传毒性剂,被认为可通过氧化途径诱导DNA损伤。我们使用彗星试验以及修复特异性酶甲酰胺基嘧啶糖基化酶(Fpg)和内切酶III(Endo III),检测了儿茶酚在人淋巴细胞和小鼠淋巴瘤细胞长期培养物中诱导DNA损伤的能力。我们的结果表明,小鼠淋巴瘤细胞对儿茶酚诱导的DNA损伤比人淋巴细胞长期培养物更敏感。在高浓度下,儿茶酚诱导的损伤似乎与Fpg和Endo III均无关,这可能表明DNA损伤存在非氧化途径(例如涉及大体积加合物)。Endo III而非Fpg增强了儿茶酚的DNA损伤作用,这一事实表明,苯的这种代谢物要么介导嘧啶而非嘌呤的氧化,要么氧化嘌呤的修复效率更高,至少在人淋巴细胞中如此。在后者细胞中,发现低浓度的儿茶酚会减少DNA迁移。考虑到Fpg的作用及其对8-氧代鸟嘌呤的加合物特异性检测,这表明低浓度的儿茶酚具有抗氧化作用,可降低氧化嘌呤的背景水平。

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