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DNA错配修复功能的丧失有助于重新激活被顺铂损伤的报告质粒。

Loss of DNA mismatch repair facilitates reactivation of a reporter plasmid damaged by cisplatin.

作者信息

Cenni B, Kim H K, Bubley G J, Aebi S, Fink D, Teicher B A, Howell S B, Christen R D

机构信息

Department of Medicine, University of California San Diego, La Jolla 92093-0058, USA.

出版信息

Br J Cancer. 1999 May;80(5-6):699-704. doi: 10.1038/sj.bjc.6690412.

Abstract

In addition to recognizing and repairing mismatched bases in DNA, the mismatch repair (MMR) system also detects cisplatin DNA adducts and loss of MMR results in resistance to cisplatin. A comparison was made of the ability of MMR-proficient and -deficient cells to remove cisplatin adducts from their genome and to reactivate a transiently transfected plasmid that had previously been inactivated by cisplatin to express the firefly luciferase enzyme. MMR deficiency due to loss of hMLH1 function did not change the extent of platinum (Pt) accumulation or kinetics of removal from total cellular DNA. However, MMR-deficient cells, lacking either hMLH1 or hMSH2, generated twofold more luciferase activity from a cisplatin-damaged reporter plasmid than their MMR-proficient counterparts. Thus, detection of the cisplatin adducts by the MMR system reduced the efficiency of reactivation of the damaged luciferase gene compared to cells lacking this detector. The twofold reduction in reactivation efficiency was of the same order of magnitude as the difference in cisplatin sensitivity between the MMR-proficient and -deficient cells. We conclude that although MMR-proficient and -deficient cells remove Pt from their genome at equal rates, the loss of a functional MMR system facilitates the reactivation of a cisplatin-damaged reporter gene.

摘要

错配修复(MMR)系统除了识别和修复DNA中错配的碱基外,还能检测顺铂DNA加合物,MMR功能丧失会导致对顺铂产生耐药性。对具备MMR功能和缺乏MMR功能的细胞从其基因组中去除顺铂加合物的能力,以及重新激活先前因顺铂失活以表达萤火虫荧光素酶的瞬时转染质粒的能力进行了比较。由于hMLH1功能丧失导致的MMR缺陷,并未改变铂(Pt)的累积程度或从总细胞DNA中去除的动力学。然而,缺乏hMLH1或hMSH2的MMR缺陷细胞,从顺铂损伤的报告质粒产生的荧光素酶活性比具备MMR功能的对应细胞多两倍。因此,与缺乏该检测功能的细胞相比,MMR系统对顺铂加合物的检测降低了受损荧光素酶基因的重新激活效率。重新激活效率降低两倍,与具备MMR功能和缺乏MMR功能的细胞之间顺铂敏感性差异处于同一数量级。我们得出结论,尽管具备MMR功能和缺乏MMR功能的细胞以相同速率从其基因组中去除Pt,但功能性MMR系统的丧失促进了顺铂损伤的报告基因的重新激活。

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