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A hit optimization protocol applied to the first nonnucleoside inhibitor of the ATPase activity of human DEAD-box RNA helicase DDX3 led to the design and synthesis of second-generation rhodanine derivatives with better inhibitory activity toward cellular DDX3 and HIV-1 replication. Additional DDX3 inhibitors were identified among triazine compounds. Biological data were rationalized in terms of structure-activity relationships and docking simulations. Antiviral activity and cytotoxicity of selected DDX3 inhibitors are reported and discussed. A thorough analysis confirmed human DDX3 as a valid anti-HIV target. The compounds described herein represent a significant advance in the pursuit of novel drugs that target HIV-1 host cofactors.

Toward the Discovery of Novel Anti-HIV Drugs. Second-Generation Inhibitors of the Cellular ATPase DDX3 with Improved Anti-HIV Activity: Synthesis, Structure-Activity Relationship Analysis, Cytotoxicity Studies, and Target Validation / Giovanni, Maga; Federico, Falchi; Radi, Marco; Lorenzo, Botta; Gianni, Casaluce; Martina, Bernardini; Hamid, Irannejad; Fabrizio, Manetti; Anna, Garbelli; Alberta, Samuele; Samantha, Zanoli; José A., Esté; Emmanuel, Gonzalez; Elisa, Zucca; Stefania, Paolucci; Fausto, Baldanti; Jan, De rijck; Zeger, Debyser; Maurizio, Botta. - In: CHEMMEDCHEM. - ISSN 1860-7179. - 6:(2011), pp. 1371-1389. [10.1002/cmdc.201100166]

Toward the Discovery of Novel Anti-HIV Drugs. Second-Generation Inhibitors of the Cellular ATPase DDX3 with Improved Anti-HIV Activity: Synthesis, Structure-Activity Relationship Analysis, Cytotoxicity Studies, and Target Validation

RADI, Marco;
2011-01-01

Abstract

A hit optimization protocol applied to the first nonnucleoside inhibitor of the ATPase activity of human DEAD-box RNA helicase DDX3 led to the design and synthesis of second-generation rhodanine derivatives with better inhibitory activity toward cellular DDX3 and HIV-1 replication. Additional DDX3 inhibitors were identified among triazine compounds. Biological data were rationalized in terms of structure-activity relationships and docking simulations. Antiviral activity and cytotoxicity of selected DDX3 inhibitors are reported and discussed. A thorough analysis confirmed human DDX3 as a valid anti-HIV target. The compounds described herein represent a significant advance in the pursuit of novel drugs that target HIV-1 host cofactors.
2011
Toward the Discovery of Novel Anti-HIV Drugs. Second-Generation Inhibitors of the Cellular ATPase DDX3 with Improved Anti-HIV Activity: Synthesis, Structure-Activity Relationship Analysis, Cytotoxicity Studies, and Target Validation / Giovanni, Maga; Federico, Falchi; Radi, Marco; Lorenzo, Botta; Gianni, Casaluce; Martina, Bernardini; Hamid, Irannejad; Fabrizio, Manetti; Anna, Garbelli; Alberta, Samuele; Samantha, Zanoli; José A., Esté; Emmanuel, Gonzalez; Elisa, Zucca; Stefania, Paolucci; Fausto, Baldanti; Jan, De rijck; Zeger, Debyser; Maurizio, Botta. - In: CHEMMEDCHEM. - ISSN 1860-7179. - 6:(2011), pp. 1371-1389. [10.1002/cmdc.201100166]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11381/2432250
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