Quinolinonyl Non-Diketo Acid Derivatives as Inhibitors of HIV-1 Ribonuclease H and Polymerase Functions of Reverse Transcriptase | Zendy

Antonella Messore | Zendy; Angela Corona | Zendy; Valentioemi Madia | Zendy; Francesco Saccoliti | Zendy; Valeria Tudino | Zendy; Alessandro De Leo | Zendy; Davide Ialongo | Zendy; Luigi Scipione | Zendy; Daniela De Vita | Zendy; Giorgio Amendola | Zendy; Ettore Novellino | Zendy; Sandro Cosconati | Zendy; Mathieu Métifiot | Zendy; MarieLine Andréola | Zendy; Francesca Esposito | Zendy; Nicole Grandi | Zendy; Enzo Tramontano | Zendy; Roberta Costi | Zendy; Roberto Di Santo | Zendy

Open Access

Quinolinonyl Non-Diketo Acid Derivatives as Inhibitors of HIV-1 Ribonuclease H and Polymerase Functions of Reverse Transcriptase

Author(s) -

Antonella Messore,

Angela Corona,

Valentioemi Madia,

Francesco Saccoliti,

Valeria Tudino,

Alessandro De Leo,

Davide Ialongo,

Luigi Scipione,

Daniela De Vita,

Giorgio Amendola,

Ettore Novellino,

Sandro Cosconati,

Mathieu Métifiot,

MarieLine Andréola,

Francesca Esposito,

Nicole Grandi,

Enzo Tramontano,

Roberta Costi,

Roberto Di Santo

Publication year - 2021

Publication title -

journal of medicinal chemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.01

H-Index - 261

eISSN - 1520-4804

pISSN - 0022-2623

DOI - 10.1021/acs.jmedchem.1c00535

Subject(s) - rnase h , reverse transcriptase , integrase , chemistry , ribonuclease , angiogenin , rnase p , enzyme , biochemistry , rnase ph , active site , polymerase , docking (animal) , stereochemistry , microbiology and biotechnology , rna , biology , dna , gene , genetics , medicine , nursing , angiogenesis

Novel anti-HIV agents are still needed to overcome resistance issues, in particular inhibitors acting against novel viral targets. The ribonuclease H (RNase H) function of the reverse transcriptase (RT) represents a validated and promising target, and no inhibitor has reached the clinical pipeline yet. Here, we present rationally designed non-diketo acid selective RNase H inhibitors (RHIs) based on the quinolinone scaffold starting from former dual integrase (IN)/RNase H quinolinonyl diketo acids. Several derivatives were synthesized and tested against RNase H and viral replication and found active at micromolar concentrations. Docking studies within the RNase H catalytic site, coupled with site-directed mutagenesis, and Mg 2+ titration experiments demonstrated that our compounds coordinate the Mg 2+ cofactor and interact with amino acids of the RNase H domain that are highly conserved among naïve and treatment-experienced patients. In general, the new inhibitors influenced also the polymerase activity of RT but were selective against RNase H vs the IN enzyme.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research