Discovery of Imidazole-Based Inhibitors of <i>Plasmodium falciparum</i> cGMP-Dependent Protein Kinase.

Bheemanaboina, Rammohan R Yadav; de Souza, Mariana Laureano; Gonzalez, Mariana Lozano; Mahmood, Shams Ul; Eck, Tyler; Kreiss, Tamara; Aylor, Samantha O; Roth, Alison; Lee, Patricia; Pybus, Brandon S; Colussi, Dennis J; Childers, Wayne E; Gordon, John; Siekierka, John J; Bhanot, Purnima; Rotella, David P

Discovery of Imidazole-Based Inhibitors of Plasmodium falciparum cGMP-Dependent Protein Kinase.

Bheemanaboina, Rammohan R Yadav; de Souza, Mariana Laureano; Gonzalez, Mariana Lozano; Mahmood, Shams Ul; Eck, Tyler; Kreiss, Tamara; Aylor, Samantha O; Roth, Alison; Lee, Patricia; Pybus, Brandon S; Colussi, Dennis J; Childers, Wayne E; Gordon, John; Siekierka, John J; Bhanot, Purnima; Rotella, David P.

Afiliação

Bheemanaboina RRY; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
de Souza ML; Department of Microbiology, Biochemistry and Molecular Genetics, Rutgers New Jersey Medical School, 225 Warren Street, Newark, New Jersey 07103, United States.
Gonzalez ML; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
Mahmood SU; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
Eck T; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
Kreiss T; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
Aylor SO; Department of Drug Discovery, Experimental Therapeutics Branch, Walter Reed Army Institute of Research, 503 Robert Grant Avenue, Silver Spring, Maryland 20910, United States.
Roth A; Department of Drug Discovery, Experimental Therapeutics Branch, Walter Reed Army Institute of Research, 503 Robert Grant Avenue, Silver Spring, Maryland 20910, United States.
Lee P; Department of Drug Discovery, Experimental Therapeutics Branch, Walter Reed Army Institute of Research, 503 Robert Grant Avenue, Silver Spring, Maryland 20910, United States.
Pybus BS; Department of Drug Discovery, Experimental Therapeutics Branch, Walter Reed Army Institute of Research, 503 Robert Grant Avenue, Silver Spring, Maryland 20910, United States.
Colussi DJ; Moulder Center for Drug Discovery Research, Temple University, Philadelphia, Pennsylvania 19140, United States.
Childers WE; Moulder Center for Drug Discovery Research, Temple University, Philadelphia, Pennsylvania 19140, United States.
Gordon J; Moulder Center for Drug Discovery Research, Temple University, Philadelphia, Pennsylvania 19140, United States.
Siekierka JJ; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.
Bhanot P; Department of Microbiology, Biochemistry and Molecular Genetics, Rutgers New Jersey Medical School, 225 Warren Street, Newark, New Jersey 07103, United States.
Rotella DP; Department of Chemistry and Biochemistry and Sokol Institute of Pharmaceutical Life Sciences, Montclair State University, Montclair, New Jersey 07043, United States.

ACS Med Chem Lett ; 12(12): 1962-1967, 2021 Dec 09.

Article em En | MEDLINE | ID: mdl-34917261

ABSTRACT

ABSTRACT

The discovery of new targets for the treatment of malaria, in particular those aimed at the pre-erythrocytic stage in the life cycle, advanced with the demonstration that orally administered inhibitors of Plasmodium falciparum cGMP-dependent protein kinase (PfPKG) could clear infection in a murine model. This enthusiasm was tempered by unsatisfactory safety and/or pharmacokinetic issues found with these chemotypes. To address the urgent need for new scaffolds, this paper presents initial structure-activity relationships in an imidazole scaffold at four positions, representative in vitro ADME, hERG characterization, and cell-based antiparasitic activity. This series of PfPKG inhibitors has good in vitro PfPKG potency, low hERG activity, and cell-based antiparasitic activity against multiple Plasmodium species that appears to be correlated with the in vitro potency.

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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2021 Tipo de documento: Article

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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2021 Tipo de documento: Article