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MutS优先识别顺铂修饰而非奥沙利铂修饰的DNA。

MutS preferentially recognizes cisplatin- over oxaliplatin-modified DNA.

作者信息

Zdraveski Zoran Z, Mello Jill A, Farinelli Christine K, Essigmann John M, Marinus Martin G

机构信息

Department of Chemistry and Division of Bioengineering and Environmental Health, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, USA.

出版信息

J Biol Chem. 2002 Jan 11;277(2):1255-60. doi: 10.1074/jbc.M105382200. Epub 2001 Nov 8.

Abstract

Loss of mismatch repair leads to tumor resistance by desensitizing cells to specific DNA-damaging agents, including the anticancer drug cisplatin. Cisplatin analogs with a diamminocyclohexane (DACH) carrier ligand, such as oxaliplatin and Pt(DACH)Cl(2), do not elicit resistance in mismatch repair-deficient cells and therefore present promising therapeutic agents. This study compared the interactions of the purified Escherichia coli mismatch repair protein MutS with DNA modified to contain cisplatin and DACH adducts. MutS recognized the cisplatin-modified DNA with 2-fold higher affinity in comparison to the DACH-modified DNA. ADP stimulated the binding of MutS to cisplatin-modified DNA, whereas it had no effect on the MutS interaction with DNA modified by DACH or EN adducts. In parallel cytotoxicity experiments, methylation-deficient E. coli dam mutants were 2-fold more sensitive to cisplatin than DACH compounds. A panel of recombination-deficient mutants showed striking sensitivity to both compounds, indicating that both types of adducts are strong replication blocks. The differential affinity of MutS for DNA modified with the different platinum analogs could provide the molecular basis for the distinctive cellular responses to cisplatin and oxaliplatin.

摘要

错配修复功能的丧失会使细胞对包括抗癌药物顺铂在内的特定DNA损伤剂产生脱敏反应,从而导致肿瘤耐药性。带有二氨基环己烷(DACH)载体配体的顺铂类似物,如奥沙利铂和Pt(DACH)Cl(2),不会在错配修复缺陷细胞中引发耐药性,因此是很有前景的治疗药物。本研究比较了纯化的大肠杆菌错配修复蛋白MutS与修饰后含有顺铂和DACH加合物的DNA之间的相互作用。与DACH修饰的DNA相比,MutS识别顺铂修饰的DNA的亲和力高2倍。ADP刺激MutS与顺铂修饰的DNA的结合,而对MutS与DACH或EN加合物修饰的DNA的相互作用没有影响。在平行的细胞毒性实验中,甲基化缺陷的大肠杆菌dam突变体对顺铂的敏感性比对DACH化合物高2倍。一组重组缺陷突变体对这两种化合物都表现出显著的敏感性,表明这两种加合物都是很强的复制障碍。MutS对用不同铂类似物修饰的DNA的不同亲和力,可能为细胞对顺铂和奥沙利铂的不同反应提供分子基础。

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