Inhibition of the self-cleavage reaction of the human hepatitis delta virus ribozyme by antibiotics

被引：127

作者：

Rogers, J ^{[1
]}

Chang, AH ^{[1
]}

vonAhsen, U ^{[1
]}

Schroeder, R ^{[1
]}

Davies, J ^{[1
]}

机构：

[1] UNIV VIENNA, INST MICROBIOL & IMMUNOL, A-1030 VIENNA, AUSTRIA

来源：

JOURNAL OF MOLECULAR BIOLOGY | 1996年 / 259卷 / 05期

关键词：

catalytic RNA; neomycin; antiviral; MgCl2; RNA footprint;

D O I：

10.1006/jmbi.1996.0369

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：

Human hepatitis delta virus (HDV) poses a health threat in populations where chronic hepatitis B is endemic. It is a single-stranded RNA virus of 1700 nucleotides and both genomic and antigenomic sequences contain ribozymes which are important for viral replication. Using ribozyme that several classes of antibiotics inhibit constructs the of the HDV ribozyme. Antibiotics of self-cleavage the aminoglycoside, peptide and tetracycline classes all inhibit HDV cleavage in vitro at micromolar concentrations. Neomycin (an aminoglycoside) inhibits HDV self-cleavage with a K-1 value of 28 (+/-10) mu M. Neomycin inhibition can be reversed by increasing magnesium ion concentration in a competitive manner. Lead acetate cleaves positions G76, A42 and G28, which surround the ribozyme cleavage site. Both Mg2+ and neomycin prevent lead cleavage. Footprinting experiments using base-specific chemical probes revealed enhanced modifications of a set of bases by neomycin, overlapping with the above mentioned lead cleavages. These observations may indicate that neomycin directly displaces divalent metal ions essential for catalysis. (C) 1996 Academic Press Limited

引用

页码：916 / 925

页数：10

共 32 条

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