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γH2Ax:DNA 修复的损伤标志物或功能参与者“并非所有闪光的都是金子!”。

γH2Ax: biomarker of damage or functional participant in DNA repair "all that glitters is not gold!".

机构信息

Department of Dermatology, University of California, San Francisco, CA, USA.

出版信息

Photochem Photobiol. 2011 Nov-Dec;87(6):1230-9. doi: 10.1111/j.1751-1097.2011.00995.x. Epub 2011 Oct 3.

Abstract

The phosphorylation of H2Ax on its S139 site, γH2Ax, is important for the assembly of repair complexes at DNA double strand breaks (DSBs). The formation and functional role of γH2Ax after other kinds of DNA damage, especially UV light, where DSBs are rare, is less clear. Following UV light in the UVB and UVC ranges, complex distributions of γH2Ax can be identified, quite unlike the discrete enumerable foci seen after ionizing radiation. Several distinct distributions of γH2Ax occur: a low level nuclear-wide distribution of γH2Ax occurs during nucleotide excision repair; irregular focal distributions occur at arrested replication forks; high intensity nuclear-wide γH2Ax occurs in association with S-phase apoptosis. The intensity and distributions of γH2Ax vary according to the activity of excision repair, bypass polymerase and apoptotic caspases. The frequency of DSBs at arrested replication forks is low but highly variable in different cell types, and probably caused by enzymatic action. Despite the prominence of S139 phosphorylation following UV damage, mutation of this site has no influence on the UV damage response indicating that γH2Ax is a biomarker but not a participant in the UV-DNA damage response.

摘要

H2Ax 在其 S139 位点的磷酸化,即 γH2Ax,对于 DNA 双链断裂 (DSB) 修复复合物的组装很重要。在其他类型的 DNA 损伤(尤其是 DSB 很少见的 UV 光)后,γH2Ax 的形成和功能作用不太清楚。在 UVB 和 UVC 范围内的 UV 光之后,可以识别到 γH2Ax 的复杂分布,与电离辐射后看到的离散可枚举焦点完全不同。有几种不同的 γH2Ax 分布:核苷酸切除修复过程中会出现低水平的核广泛 γH2Ax 分布;停滞复制叉处会出现不规则的焦点分布;与 S 期细胞凋亡相关的核广泛 γH2Ax 会出现高强度分布。γH2Ax 的强度和分布根据切除修复、旁路聚合酶和凋亡半胱氨酸蛋白酶的活性而变化。停滞复制叉处 DSB 的频率较低,但在不同细胞类型中变化很大,可能是由酶的作用引起的。尽管 S139 磷酸化在 UV 损伤后很明显,但该位点的突变对 UV 损伤反应没有影响,这表明 γH2Ax 是一个生物标志物,但不是 UV-DNA 损伤反应的参与者。

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