DNA-SUBSTRATE SEQUENCE SPECIFICITY OF HUMAN G-T MISMATCH REPAIR ACTIVITY

被引：21

作者：

SIBGHATULLAH ^{[1
]}

DAY, RS ^{[1
]}

机构：

[1] CROSS CANC INST, DEPT MED, MOLEC ONCOL PROGRAM, 11560 UNIV AVE, EDMONTON T6G 1Z2, ALBERTA, CANADA

来源：

NUCLEIC ACIDS RESEARCH | 1993年 / 21卷 / 05期

关键词：

D O I：

10.1093/nar/21.5.1281

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

G:T mispairs in DNA originate spontaneously via deamination of 5-methylcytosine. Such mispairs are restored to normal G:C pairs by both E.coli K strains and human cells. In this study we have analyzed the repair by human cell extracts of G:T mismatches in various DNA contexts. We performed two sets of experiments. In the first, repair was sequence specific in that G:T mispairs at CpG sites at four different CpG sites were repaired, but a G:T mismatch at a GpG site was not. Cytosine hemimethylation did not block repair of a substrate containing a CpG/GpT mismatch. In the second set of experiments, substrates with a G:T mismatch at a fixed position were constructed with an A, T, G, or C 5' to the mismatched G, and alterations in the complementary strand to allow otherwise perfect Watson-Crick pairing. All were incised just 5' to the mismatched T and competed for repair incision with a G:T substrate in which a C was 5' to the mismatched G. Thus human G:T mismatch activity shows sequence specificity, incising G:T mismatched pairs at some DNA sites, but not at others. At an incisable site, however, incision is little influenced by the base 5' to the mismatched G.

引用

页码：1281 / 1287

页数：7

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