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铂类抗癌药物损伤会强制使核小体中DNA处于特定的旋转状态。

Platinum anticancer drug damage enforces a particular rotational setting of DNA in nucleosomes.

作者信息

Danford Andrew J, Wang Dong, Wang Qun, Tullius Thomas D, Lippard Stephen J

机构信息

Department of Chemistry, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 2005 Aug 30;102(35):12311-6. doi: 10.1073/pnas.0506025102. Epub 2005 Aug 22.

Abstract

We constructed two site-specifically modified nucleosomes containing an intrastrand cis-{Pt(NH3)2}2+ 1,3-d(GpTpG) cross-link, similar to one formed by the anticancer drugs carboplatin and cisplatin on DNA, and investigated their structures by hydroxyl radical footprinting and exonuclease III digestion. Hydroxyl radical footprinting demonstrated that the presence of the platinum cross-link selects out a specific rotational setting of DNA on the histone octamer core in each of two reconstituted nucleosomes in which the platinum positions differ by half a DNA helical turn. The {Pt(NH3)2}2+ cross-link is situated in a structurally similar location, with the undamaged strand projecting outward, forcing the DNA to adopt opposite rotational settings in its wrapping around the histone octamer in the two nucleosomes. Enzymatic digestion by exonuclease III of the nucleosome substrates revealed that the platinum cross-link affects the translational positioning of the DNA, forcing it into an asymmetric arrangement with respect to the core histone proteins. We suggest that these phasing phenomena may be central to the recognition and processing of platinum-DNA adducts in cancer cells treated with these drugs and possibly may be common to other DNA damaging events.

摘要

我们构建了两个位点特异性修饰的核小体,其中含有链内顺式-{Pt(NH3)2}2+ 1,3-d(GpTpG)交联,类似于抗癌药物卡铂和顺铂在DNA上形成的交联,并通过羟基自由基足迹法和核酸外切酶III消化研究了它们的结构。羟基自由基足迹法表明,铂交联的存在在两个重构核小体的每一个中选择了DNA在组蛋白八聚体核心上的特定旋转设置,其中铂的位置相差半个DNA螺旋圈。{Pt(NH3)2}2+交联位于结构相似的位置,未受损的链向外突出,迫使DNA在围绕两个核小体中的组蛋白八聚体缠绕时采用相反的旋转设置。核酸外切酶III对核小体底物的酶切消化表明,铂交联影响DNA的平移定位,使其相对于核心组蛋白形成不对称排列。我们认为,这些相位现象可能是在用这些药物治疗的癌细胞中识别和处理铂-DNA加合物的核心,并且可能是其他DNA损伤事件所共有的。

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