Unusual binding mode of an HIV-1 protease inhibitor explains its potency against multi-drug-resistant virus strains
Jazyk angličtina Země Nizozemsko Médium print
Typ dokumentu časopisecké články, práce podpořená grantem
PubMed
12460574
DOI
10.1016/s0022-2836(02)01139-7
PII: S0022283602011397
Knihovny.cz E-zdroje
- MeSH
- antibiotická rezistence genetika MeSH
- genotyp MeSH
- HIV infekce farmakoterapie virologie MeSH
- HIV-1 účinky léků genetika metabolismus MeSH
- inhibitory HIV-proteasy chemie metabolismus farmakologie MeSH
- inhibitory reverzní transkriptasy farmakologie MeSH
- kinetika MeSH
- konformace proteinů MeSH
- krystalografie rentgenová MeSH
- lidé MeSH
- mnohočetná léková rezistence genetika MeSH
- molekulární konformace MeSH
- molekulární modely MeSH
- molekulární struktura MeSH
- mutace MeSH
- oligopeptidy chemie metabolismus farmakologie MeSH
- proteinové inženýrství MeSH
- racionální návrh léčiv MeSH
- rekombinantní proteiny chemie izolace a purifikace metabolismus MeSH
- substituce aminokyselin MeSH
- vazebná místa MeSH
- vysoce aktivní antiretrovirová terapie MeSH
- Check Tag
- lidé MeSH
- mužské pohlaví MeSH
- ženské pohlaví MeSH
- Publikační typ
- časopisecké články MeSH
- práce podpořená grantem MeSH
- Názvy látek
- inhibitory HIV-proteasy MeSH
- inhibitory reverzní transkriptasy MeSH
- oligopeptidy MeSH
- QF34 pseudopeptide MeSH Prohlížeč
- rekombinantní proteiny MeSH
Protease inhibitors (PIs) are an important class of drugs for the treatment of HIV infection. However, in the course of treatment, resistant viral variants with reduced sensitivity to PIs often emerge and become a major obstacle to successful control of viral load. On the basis of a compound equipotently inhibiting HIV-1 and 2 proteases (PR), we have designed a pseudopeptide inhibitor, QF34, that efficiently inhibits a wide variety of PR variants. In order to analyze the potency of the inhibitor, we constructed PR species harboring the typical (signature) mutations that confer resistance to commercially available PIs. Kinetic analyses showed that these mutated PRs were inhibited up to 1,000-fold less efficiently by the clinically approved PIs. In contrast, all PR species were effectively inhibited by QF34. In a clinical study, we have monitored 30 HIV-positive patients in the Czech Republic undergoing highly active antiretroviral therapy, and have identified highly PI resistant variants. Kinetic analyses revealed that QF34 retained its subnanomolar potency against multi-drug resistant PR variants. X-ray crystallographic analysis and molecular modeling experiments explained the wide specificity of QF34: this inhibitor binds to the PR in an unusual manner, thus avoiding contact sites that are mutated upon resistance development, and the unusual binding mode and consequently the binding energy is therefore preserved in the complex with a resistant variant. These results suggest a promising route for the design of second-generation PIs that are active against a variety of resistant PR variants.
Citace poskytuje Crossref.org
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