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紫外线照射的人类细胞中修复的抑制作用。

The inhibition of repair in UV irradiated human cells.

作者信息

Collins A R, Schor S L, Johnson R T

出版信息

Mutat Res. 1977 Mar;42(3):413-32. doi: 10.1016/s0027-5107(77)80046-8.

Abstract

We have used three different assay procedures to determine the effects of hydroxyurea on excision repair in UV-irradiated HeLa cells. The results were as follows. (a) At the cytological level, incubation of UV-irradiated metaphase cells with hydroxyurea caused chromosome decondensation. (b) Using a modified alkaline sucrose gradient sedimentation technique involving minimal lysis before centrifugation, we found a marked retardation in the sedimentation of DNA from UV-irradiated cells incubated for a short period with hydroxyurea. (c) The effect of hydroxyurea on the incorporation of[3H]thymidine by UV-irradiated G1 cells was found to depend on the concentration of thymidine present in the medium. Normal primary human cells resemble HeLa cells in the response of chromosomes and DNA to UV plus hydroxyurea. Xeroderma pigmentosum cells, deficient in excision repair, are not sensitive to hydroxyurea in our assays. Chromosome decondensation and retarded DNA sedimentation occur also after incubation of irradiated HeLa cells with deoxyadenosine, but not thymidine, at concentrations which inhibit semiconservative DNA synthesis. The effects of hydroxyurea or deoxyadenosine on chromosomes and DNA are not seen if all four deoxyribonucleoside precursors of DNA are supplied exogenously. These results point to an inhibition of repair DNA synthesis by hydroxyurea (or deoxyadenosine), at the level of the supply of DNA precursors, i.e. in the same way that these agents inhibit semiconservative DNA synthesis. In the presence of these inhibitors, single-strand gaps accumulate in the DNA.

摘要

我们采用了三种不同的检测方法来确定羟基脲对紫外线照射的HeLa细胞中切除修复的影响。结果如下:(a) 在细胞学水平上,用羟基脲孵育紫外线照射的中期细胞会导致染色体解聚。(b) 使用一种改良的碱性蔗糖梯度沉降技术,即在离心前尽量减少细胞裂解,我们发现,用羟基脲短期孵育的紫外线照射细胞的DNA沉降明显延迟。(c) 发现羟基脲对紫外线照射的G1期细胞掺入[3H]胸腺嘧啶的影响取决于培养基中胸腺嘧啶的浓度。正常原代人细胞在染色体和DNA对紫外线加羟基脲的反应方面与HeLa细胞相似。在我们的检测中,缺乏切除修复能力的着色性干皮病细胞对羟基脲不敏感。用脱氧腺苷而非胸腺嘧啶孵育照射后的HeLa细胞,在抑制半保留DNA合成的浓度下,也会出现染色体解聚和DNA沉降延迟的情况。如果从外源提供DNA的所有四种脱氧核糖核苷前体,则看不到羟基脲或脱氧腺苷对染色体和DNA的影响。这些结果表明,羟基脲(或脱氧腺苷)在DNA前体供应水平上抑制修复性DNA合成,即与这些试剂抑制半保留DNA合成的方式相同。在这些抑制剂存在的情况下,DNA中会积累单链缺口。

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