TRIPLE-HELIX FORMATION WITH SHORT OLIGONUCLEOTIDE INTERCALATOR CONJUGATES MATCHING THE HIV-1 U3 LTR END SEQUENCE

被引：59

作者：

MOUSCADET, JF ^{[1
]}

KETTERLE, C ^{[1
]}

GOULAOUIC, H ^{[1
]}

CARTEAU, S ^{[1
]}

SUBRA, F ^{[1
]}

LEBRET, M ^{[1
]}

AUCLAIR, C ^{[1
]}

机构：

[1] INST GUSTAVE ROUSSY, PHYSICOCHIM & PHARMACOL MACROMOLEC BIOL LAB,CNRS, URA 147,INSERM, F-94805 VILLEJUIF, FRANCE

来源：

BIOCHEMISTRY | 1994年 / 33卷 / 14期

关键词：

D O I：

10.1021/bi00180a011

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：

In an attempt to target short purine sequences in view of pharmacological application, we have synthesized three new TFO (triple-helix-forming oligonucleotide) conjugates in which an intercalating oxazolopyridocarbazole (OPC) chromophore is linked by a pentamethylene linker to a 7-mer oligonucleotide matching the polypurine/polypyrimidine sequence located in the HIV-1 U3 LTR end region. The TFO moiety of conjugates are 5'CCTTCCC, 5'GGGAAGG, and 5'GGGTTGG. Their ability to bind to double-stranded DNA targets was examined. This binding- is demonstrated by a footprinting technique using DNase I as a cleaving agent. The complex involved intermolecular pyr-purpyr or pur-purpyr triple helix. Pyrimidine TFO-OPC binds in a pH-dependent manner, whereas the others do not. The formation of the complex has been investigated at neutral pH and increasing temperature. We observed that the protection due to the purine and mixed TFO-OPC was pH independent and remained identical up to 40-degrees-C. To determine the position of the OPC chromophore, molecular modeling was undertaken on the purine-conjugate/target complex. It has been suggested that the complex involved the intercalation of the OPC at the triplex-duplex junction with a small unwinding at the next excluded site.

引用

页码：4187 / 4196

页数：10

共 54 条

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