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首页> 美国卫生研究院文献>Cell Death Discovery >Induction and inhibition of the pan-nuclear gamma-H2AX response in resting human peripheral blood lymphocytes after X-ray irradiation
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Induction and inhibition of the pan-nuclear gamma-H2AX response in resting human peripheral blood lymphocytes after X-ray irradiation

机译:X射线照射后静息人外周血淋巴细胞中泛核γ-H2AX反应的诱导和抑制

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Human peripheral blood lymphocytes (HPBLs) are one of the most sensitive cells to ionizing radiation (IR) in the human body, and IR-induced DNA damage and functional impairment of HPBLs are the adverse consequences of IR accidents and major side effects of radiotherapy. Phosphorylated H2AX (γH2AX) is a sensitive marker for DNA double-strand breaks, but the role and regulation of the pan-nuclear γH2AX response in HPBLs after IR remain unclear. We herein demonstrated that the pan-nuclear γH2AX signals were increased in a time- and dose-dependent manner, colocalized with >94% of TUNEL apoptotic staining, and displayed a typical apoptotic pattern in resting HPBLs after low LET X-ray IR. In addition, the X-irradiation-induced pan-nuclear p-ATM and p-DNA-PKcs responses also occurred in resting HPBLs, and were colocalized with 92–95% of TUNEL staining and 97–98% of the pan-nuclear γH2AX signals, respectively, with a maximum at 6 h post irradiation, but disappeared at 24 h post irradiation. Moreover, ATM/DNA-PKcs inhibitor KU55933, p53 inhibitor PFT-μ and pan-caspase inhibitor ZVAD-fmk significantly decreased X-irradiation-induced pan-nuclear γH2AX signals and TUNEL staining, protected HPBLs from apoptosis, but decreased the proliferative response to mitogen in X-irradiated HPBLs. Notably, whereas both KU55933 and PFT-μ increased the IR-induced chromosome breaks and mis-repair events through inhibiting the formation of p-ATM, p-DNA-PKcs and γH2AX foci in X-irradiated HPBLs, the ZVAD-fmk did not increase the IR-induced chromosomal instability. Taken together, our data indicate that pan-nuclear γH2AX response represents an apoptotic signal that is triggered by the transient pan-nuclear ATM and DNA-PKcs activation, and mediated by p53 and pan-caspases in X-irradiated HPBLs, and that caspase inhibitors are better than ATM/DNA-PKcs inhibitors and p53 inhibitors to block pan-nuclear γH2AX response/apoptosis and protect HPBLs from IR.
机译:人外周血淋巴细胞(HPBL)是对人体中电离辐射(IR)最敏感的细胞之一,IR诱导的DNA损伤和HPBLs的功能受损是IR事故和放射疗法的主要副作用的不良后果。磷酸化的H2AX(γH2AX)是DNA双链断裂的敏感标记,但是IR后在HPBLs中泛核γH2AX反应的作用和调节尚不清楚。我们在本文中证明,泛核γH2AX信号以时间和剂量依赖性方式增加,与> 94%的TUNEL细胞凋亡染色共定位,并在低LET X射线IR后在静止的HPBLs中显示典型的细胞凋亡模式。此外,X射线诱导的全核p-ATM和p-DNA-PKcs反应也发生在静止的HPBLs中,并且与92-95%的TUNEL染色和97-98%的全核γH2AX共同定位信号分别在辐照后6 h达到最大值,但在辐照后24 h消失。此外,ATM / DNA-PKcs抑制剂KU55933,p53抑制剂PFT-μ和泛半胱天冬酶抑制剂ZVAD-fmk显着降低了X射线诱导的泛核γH2AX信号和TUNEL染色,保护了HPBLs免受凋亡,但降低了对X射线照射的HPBLs中有丝分裂原。值得注意的是,尽管KU55933和PFT-μ都通过抑制X射线照射的HPBL中p-ATM,p-DNA-PKcs和γH2AX灶的形成而增加了IR诱导的染色体断裂和错误修复事件,但ZVAD-fmk却没有增加IR引起的染色体不稳定性。两者合计,我们的数据表明泛核γH2AX反应代表凋亡信号,该信号由瞬时泛核ATM和DNA-PKcs激活触发,并由X射线照射的HPBLs中的p53和泛半胱天冬酶介导,并且胱天蛋白酶抑制剂与ATM / DNA-PKcs抑制剂和p53抑制剂相比,它们在阻断泛核γH2AX反应/凋亡和保护HPBL免受IR侵袭方面更胜一筹。

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