SITE-DEPENDENT INHIBITION BY SINGLE O6-METHYLGUANINE BASES OF SV40 T-ANTIGEN INTERACTIONS WITH THE VIRAL ORIGIN OF REPLICATION

被引:8
作者
BIGNAMI, M [1 ]
KARRAN, P [1 ]
LANE, DP [1 ]
机构
[1] IMPERIAL CANC RES FUND,CLARE HALL LABS,S MIMMS EN6 3LD,HERTS,ENGLAND
来源
BIOCHEMISTRY | 1991年 / 30卷 / 11期
关键词
D O I
10.1021/bi00225a018
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
The effects of O6-methylguanine on the reactions involved in initiation of DNA replication were investigated by measuring the interactions of SV40 T antigen with oligonucleotides substituted with the methylated base. O6-Methylguanine residues were positioned in either binding site I or binding site II of the SV40 origin of replication. Binding of purified T antigen, measured by both nitrocellulose filter binding and delayed oligonucleotide migration, was unaffected by the presence of seven methylated bases in binding site II. Single substitutions within binding site I were sufficient to inhibit T-antigen binding, and the extent of inhibition was dependent on the position of O6-methylguanine in the DNA sequence. Unwinding by T antigen was analyzed by measuring displacement of a single-stranded oligonucleotide from similarly substituted, partially duplex substrates. The presence of three O6-methylguanine residues in binding site I facilitated the helicase activity of T antigen. In contrast, single O6-methylguanine bases inhibited unwinding. A correlation was observed between the position of the methylated base and the inhibition of both binding and unwinding by T antigen.
引用
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页码:2857 / 2863
页数:7
相关论文
共 38 条
[1]  
AQUILINA G, 1990, CANCER RES, V50, P4248
[2]   O-6-METHYLGUANINE IN THE SV40 ORIGIN OF REPLICATION INHIBITS BINDING BUT INCREASES UNWINDING BY VIRAL LARGE T-ANTIGEN [J].
BIGNAMI, M ;
LANE, DP .
NUCLEIC ACIDS RESEARCH, 1990, 18 (13) :3785-3793
[3]   ATP STIMULATES THE BINDING OF SIMIAN VIRUS-40 (SV40) LARGE TUMOR-ANTIGEN TO THE SV40 ORIGIN OF REPLICATION [J].
BOROWIEC, JA ;
HURWITZ, J .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (01) :64-68
[4]   IDENTIFICATION OF AN ORIGIN OF BIDIRECTIONAL DNA-REPLICATION IN MAMMALIAN CHROMOSOMES [J].
BURHANS, WC ;
VASSILEV, LT ;
CADDLE, MS ;
HEINTZ, NH ;
DEPAMPHILIS, ML .
CELL, 1990, 62 (05) :955-965
[5]  
CHALLBERG MD, 1989, ANNU REV BIOCHEM, V58, P671
[6]  
CROTHERS DM, 1990, J BIOL CHEM, V265, P7093
[7]   DEFECTIVE REPAIR OF ALKYLATED DNA BY HUMAN-TUMOR AND SV40-TRANSFORMED HUMAN CELL STRAINS [J].
DAY, RS ;
ZIOLKOWSKI, CHJ ;
SCUDIERO, DA ;
MEYER, SA ;
LUBINIECKI, AS ;
GIRARDI, AJ ;
GALLOWAY, SM ;
BYNUM, GD .
NATURE, 1980, 288 (5792) :724-727
[8]   ATP-DEPENDENT FORMATION OF A SPECIALIZED NUCLEOPROTEIN STRUCTURE BY SIMIAN VIRUS-40 (SV40) LARGE TUMOR-ANTIGEN AT THE SV40 REPLICATION ORIGIN [J].
DEAN, FB ;
DODSON, M ;
ECHOLS, H ;
HURWITZ, J .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (24) :8981-8985
[9]   DOMAIN-STRUCTURE OF THE SIMIAN VIRUS-40 CORE ORIGIN OF REPLICATION [J].
DEB, S ;
DELUCIA, AL ;
BAUR, CP ;
KOFF, A ;
TEGTMEYER, P .
MOLECULAR AND CELLULAR BIOLOGY, 1986, 6 (05) :1663-1670
[10]   THE T-ANTIGEN-BINDING DOMAIN OF THE SIMIAN VIRUS-40 CORE ORIGIN OF REPLICATION [J].
DEB, S ;
TSUI, S ;
KOFF, A ;
DELUCIA, AL ;
PARSONS, R ;
TEGTMEYER, P .
JOURNAL OF VIROLOGY, 1987, 61 (07) :2143-2149
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