Characterization and in vitro activity of a branched peptide boronic acid that interacts with HIV-1 RRE RNA

Characterization and in vitro activity of a branched peptide boronic acid that interacts with HIV-1 RRE RNA

[Display omitted] A branched peptide containing multiple boronic acids was found to bind RRE IIB selectively and inhibit HIV-1 p24 capsid production in a dose-dependent manner. Structure–activity relationship studies revealed that branching in the peptide is crucial for the low micromolar binding to...

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Veröffentlicht in:Bioorganic & medicinal chemistry 2016-09, Vol.24 (17), p.3947-3952
Hauptverfasser: Wynn, Jessica E., Zhang, Wenyu, Tebit, Denis M., Gray, Laurie R., Hammarskjold, Marie-Louise, Rekosh, David, Santos, Webster L.
Format: Artikel
Sprache:eng
Schlagworte:
Anti-HIV Agents - chemistry
Anti-HIV Agents - pharmacology
Boronic acids
Boronic Acids - chemistry
Boronic Acids - pharmacology
Branched peptides
HeLa Cells
HIV Core Protein p24 - antagonists & inhibitors
HIV-1
HIV-1 - drug effects
HIV-1 - genetics
Humans
Integrase Inhibitors - pharmacology
Lamivudine - pharmacology
Nucleic Acid Conformation
p24 inhibition
Peptide Library
Peptides - chemistry
Peptides - pharmacology
Quinolones - pharmacology
Raltegravir Potassium - pharmacology
Response Elements
RNA, Viral - chemistry
RNA, Viral - genetics
RNA, Viral - metabolism
RRE RNA
Structure-Activity Relationship
Virus Replication - drug effects
Zidovudine - pharmacology
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Zusammenfassung:[Display omitted] A branched peptide containing multiple boronic acids was found to bind RRE IIB selectively and inhibit HIV-1 p24 capsid production in a dose-dependent manner. Structure–activity relationship studies revealed that branching in the peptide is crucial for the low micromolar binding towards RRE IIB, and the peptide demonstrates selectivity towards RRE IIB in the presence of tRNA. Footprinting studies suggest a binding site on the upper stem and internal loop regions of the RNA, which induces enzymatic cleavage of the internal loops of RRE IIB upon binding.
ISSN:0968-0896
1464-3391
DOI:10.1016/j.bmc.2016.04.009