Functional and Structural Characterization of 2‑Amino-4-phenylthiazole Inhibitors of the HIV‑1 Nucleocapsid Protein with Antiviral Activity

The nucleocapsid protein (NC) is a highly conserved protein in diverse HIV-1 subtypes that plays a central role in virus replication, mainly by interacting with conserved nucleic acid sequences. NC is considered a highly profitable drug target to inhibit multiple steps in the HIV-1 life cycle with j...

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Veröffentlicht in:ACS chemical biology 2014-09, Vol.9 (9), p.1950-1955
Hauptverfasser: Mori, Mattia, Nucci, Alessandro, Lang, Maria Chiara Dasso, Humbert, Nicolas, Boudier, Christian, Debaene, Francois, Sanglier-Cianferani, Sarah, Catala, Marjorie, Schult-Dietrich, Patricia, Dietrich, Ursula, Tisné, Carine, Mely, Yves, Botta, Maurizio
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Sprache:eng
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Zusammenfassung:The nucleocapsid protein (NC) is a highly conserved protein in diverse HIV-1 subtypes that plays a central role in virus replication, mainly by interacting with conserved nucleic acid sequences. NC is considered a highly profitable drug target to inhibit multiple steps in the HIV-1 life cycle with just one compound, a unique property not shown by any of the other antiretroviral classes. However, most of NC inhibitors developed so far act through an unspecific and potentially toxic mechanism (zinc ejection) and are mainly being investigated as topical microbicides. In an effort to provide specific NC inhibitors that compete for the binding of nucleic acids to NC, here we combined molecular modeling, organic synthesis, biophysical studies, NMR spectroscopy, and antiviral assays to design, synthesize, and characterize an efficient NC inhibitor endowed with antiviral activity in vitro, a desirable property for the development of efficient antiretroviral lead compounds.
ISSN:1554-8929
1554-8937
DOI:10.1021/cb500316h