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同步化二倍体人成纤维细胞S期的DNA损伤检查点反应

DNA damage checkpoint responses in the S phase of synchronized diploid human fibroblasts.

作者信息

Chastain Paul D, Brylawski Bruna P, Zhou Yingchun C, Rao Shangbang, Chu Haitao, Ibrahim Joseph G, Kaufmann William K, Cordeiro-Stone Marila

机构信息

College of Osteopathic Medicine, William Carey University, Hattiesburg, MS.

出版信息

Photochem Photobiol. 2015 Jan-Feb;91(1):109-16. doi: 10.1111/php.12361. Epub 2014 Nov 24.

Abstract

We investigated the hypothesis that the strength of the activation of the intra-S DNA damage checkpoint varies within the S phase. Synchronized diploid human fibroblasts were exposed to either 0 or 2.5 J m(-2) UVC in early, mid- and late-S phase. The endpoints measured were the following: (1) radio-resistant DNA synthesis (RDS), (2) induction of Chk1 phosphorylation, (3) initiation of new replicons and (4) length of replication tracks synthesized after irradiation. RDS analysis showed that global DNA synthesis was inhibited by approximately the same extent (30 ± 12%), regardless of when during S phase the fibroblasts were exposed to UVC. Western blot analysis revealed that the UVC-induced phosphorylation of checkpoint kinase 1 (Chk1) on serine 345 was high in early and mid S but 10-fold lower in late S. DNA fiber immunostaining studies indicated that the replication fork displacement rate decreased in irradiated cells at the three time points examined; however, replicon initiation was inhibited strongly in early and mid S, but this response was attenuated in late S. These results suggest that the intra-S checkpoint activated by UVC-induced DNA damage is not as robust toward the end of S phase in its inhibition of the latest firing origins in human fibroblasts.

摘要

我们研究了一个假说,即S期内DNA损伤检查点的激活强度在S期内是变化的。将同步化的二倍体人成纤维细胞在S期早期、中期和晚期分别暴露于0或2.5 J m(-2) 的紫外线C(UVC)。所测量的终点指标如下:(1)抗辐射DNA合成(RDS),(2)Chk1磷酸化的诱导,(3)新复制子的起始,以及(4)照射后合成的复制轨道长度。RDS分析表明,无论成纤维细胞在S期的何时暴露于UVC,总体DNA合成均受到大致相同程度(30±12%)的抑制。蛋白质印迹分析显示,UVC诱导的检查点激酶1(Chk1)丝氨酸345位点的磷酸化在S期早期和中期较高,但在S期晚期低10倍。DNA纤维免疫染色研究表明,在检测的三个时间点,照射细胞中的复制叉移动速率均降低;然而,复制子起始在S期早期和中期受到强烈抑制,但这种反应在S期晚期减弱。这些结果表明,由UVC诱导的DNA损伤激活S期内检查点在抑制人成纤维细胞中最晚起始的复制起点方面,在S期末期的作用不如早期和中期强大。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4cf2/4303954/476bda108cb2/php0091-0109-f1.jpg

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