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Caffeine and human DNA metabolism: the magic and the mystery

机译:咖啡因与人类DNA代谢:魔力与奥秘

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摘要

The ability of caffeine to reverse cell cycle checkpoint function and enhance genotoxicity after DNA damage was examined in telomerase-expressing human fibroblasts. Caffeine reversed the ATM-dependent S and G2 checkpoint responses to DNA damage induced by ionizing radiation (IR), as well as the ATR- and Chk1-dependent S checkpoint response to ultraviolet radiation (UVC). Remarkably, under conditions in which IR-induced G2 delay was reversed by caffeine, IR-induced G1 arrest was not. Incubation in caffeine did not increase the percentage of cells entering the S phase 6–8 h after irradiation; ATM-dependent phosphorylation of p53 and transactivation of p21Cip1/Waf1 post-IR were resistant to caffeine. Caffeine alone induced a concentration- and time-dependent inhibition of DNA synthesis. It inhibited the entry of human fibroblasts into S phase by 70–80% regardless of the presence or absence of wildtype ATM or p53. Caffeine also enhanced the inhibition of cell proliferation induced by UVC in XP variant fibroblasts. This effect was reversed by expression of DNA polymerase η, indicating that translesion synthesis of UVC-induced pyrimidine dimers by DNA pol η protects human fibroblasts against UVC genotoxic effects even when other DNA repair functions are compromised by caffeine.
机译:在表达端粒酶的人类成纤维细胞中检查了咖啡因逆转细胞周期检查点功能和增强DNA损伤后的遗传毒性的能力。咖啡因逆转了ATM依赖的S和G2检查点对电离辐射(IR)引起的DNA损伤的响应,以及ATR和Chk1依赖的S检查点对紫外线(UVC)的响应。值得注意的是,在咖啡因逆转了IR诱导的G2延迟的条件下,IR诱导的G1阻滞却没有。在咖啡因中孵育不会增加辐射后6-8小时进入S期的细胞的百分比; IR后p53的ATM依赖性磷酸化和p21 Cip1 / Waf1 的反式激活对咖啡因具有抗性。单独的咖啡因会引起浓度和时间依赖性的DNA合成抑制。无论是否存在野生型ATM或p53,它都能将人成纤维细胞进入S期的抑制率达70-80%。咖啡因还可以增强XP变异成纤维细胞中UVC诱导的细胞增殖抑制作用。 DNA聚合酶η的表达逆转了这种效应,表明DNA polη的UVC诱导的嘧啶二聚体的反转录合成可保护人成纤维细胞免受UVC的遗传毒性影响,即使咖啡因损害了其他DNA修复功能。

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