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TRIPLE-HELIX FORMATION IS COMPATIBLE WITH AN ADJACENT DNA PROTEIN COMPLEX
被引:7
|作者:
HUANG, CC
NGUYEN, D
MARTINEZ, R
EDWARDS, CA
机构:
[1] GENELABS INC,DRUG DISCOVERY SYST RES GRP,505 PENOBSCOT DR,REDWOOD CITY,CA 94063
[2] GENELABS INC,MOLEC VIROL GRP,REDWOOD CITY,CA 94063
关键词:
D O I:
10.1021/bi00119a007
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 effect of oligonucleotide-directed triple-helix formation on the binding of a protein to an immediately adjacent sequence has been examined. A double-stranded oligonucleotide was designed with a target site for the binding of a pyrimidine oligonucleotide located immediately adjacent to the recognition sequence for the herpes simplex virus type 1 (HSV-1) origin of replication binding protein, which is encoded by the UL9 gene of HSV-1. Since the optimal conditions for the binding of the UL9 protein and the pyrimidine oligonucleotide to the duplex DNA are markedly different, a pyrimidine oligonucleotide was designed to optimize binding affinity and specificity for the target duplex oligonucleotide. Consideration was given to length and sequence composition in an effort to maximize triple-strand formation under conditions amenable to the formation of the UL9-DNA complex. Using gel mobility shift assays, a trimolecular complex composed of duplex DNA bound to both a third oligonucleotide strand and the UL9 protein was detected, indicating that the UL9-DNA complex is compatible with the presence of a triple helix in the immediately adjacent sequences.
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页码:993 / 998
页数:6
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