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γ-H2AX/53BP1/pKAP-1 foci and their linear tracks induced by in vitro exposure to radon and its progeny in human peripheral blood lymphocytes

机译:体外暴露于人外周血淋巴细胞中的and及其子代后诱导的γ-H2AX/ 53BP1 / pKAP-1基因座及其线性轨迹

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The biodosimetric information is critical for evaluating the human health hazards caused by radon and its progeny. Here, we demonstrated that the formation of phosphorylated histone variant H2AX (γ-H2AX), p53-binding protein 1 (53BP1) and phosphorylated KRAB-associated protein 1 (pKAP-1) foci and their linear tracks in human peripheral blood lymphocytes (HPBLs) in vitro exposed to radon and its progeny were dependent on the cumulative absorbed dose of radon exposure but was unrelated to the concentration of radon. Among them, γ-H2AX foci and its linear tracks were the most sensitive indicators with the lowest estimable cumulative absorbed dose of 1.74 mGy from their linear dose-response curves and sustained for 12?h after termination of radon exposure. In addition, three types of foci showed an overdispersed non-Poisson distribution in HPBLs. The ratios of pKAP-1/γ-H2AX foci co-localization, 53BP1/γ-H2AX foci co-localization and 53BP1/pKAP-1 foci co-localization were significantly increased in HPBLs exposed to radon while they were unrelated to the cumulative dose of radon exposure, suggesting that γ-H2AX, pKAP-1 and 53BP1 play an important role in the repair of heterochromatic double-strand breaks. Altogether, our findings provide an experimental basis for estimating the biological dose of internal α-particle irradiation from radon and its progeny exposure in humans.
机译:生物剂量学信息对于评估by及其后代对人体健康的危害至关重要。在这里,我们证明了在人外周血淋巴细胞(HPBLs)中磷酸化组蛋白变体H2AX(γ-H2AX),p53结合蛋白1(53BP1)和磷酸化KRAB相关蛋白1(pKAP-1)的形成及其线性轨迹)体外暴露于ra及其子代取决于on暴露的累积吸收剂量,但与of浓度无关。其中,γ-H2AX病灶及其线性径迹是最敏感的指示剂,从其线性剂量反应曲线可估计的最低累积吸收剂量为1.74 mGy,并在termination暴露终止后持续12?h。此外,三种类型的病灶在HPBLs中显示出非泊松分布过度分散。在暴露于ra的HPBLs中,pKAP-1 /γ-H2AX灶共定位,53BP1 /γ-H2AX灶共定位和53BP1 / pKAP-1灶共定位的比率显着增加,而与累积剂量无关ra暴露,表明γ-H2AX,pKAP-1和53BP1在修复异色双链断裂中起重要作用。总之,我们的发现为估算provide中内部α粒子辐射的生物剂量及其后代在人体内的暴露提供了实验基础。

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