A Sub-Micromolar MraYAA Inhibitor with an Aminoribosyl Uridine Structure and a (S,S)-Tartaric Diamide: Synthesis, Biological Evaluation and Molecular Modeling.

Oliver, Martin; Le Corre, Laurent; Poinsot, Mélanie; Bosco, Michaël; Wan, Hongwei; Amoroso, Ana; Joris, Bernard; Bouhss, Ahmed; Calvet-Vitale, Sandrine; Gravier-Pelletier, Christine

A Sub-Micromolar MraY_AA Inhibitor with an Aminoribosyl Uridine Structure and a (S,S)-Tartaric Diamide: Synthesis, Biological Evaluation and Molecular Modeling.

Oliver, Martin; Le Corre, Laurent; Poinsot, Mélanie; Bosco, Michaël; Wan, Hongwei; Amoroso, Ana; Joris, Bernard; Bouhss, Ahmed; Calvet-Vitale, Sandrine; Gravier-Pelletier, Christine.

Afiliación

Oliver M; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Le Corre L; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Poinsot M; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Bosco M; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Wan H; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Amoroso A; Unité de Physiologie et Génétique Bactériennes, Centre d'Ingénierie des Protéines, Département des Sciences de la Vie, Université de Liège, Sart Tilman, B4000 Liège, Belgium.
Joris B; Unité de Physiologie et Génétique Bactériennes, Centre d'Ingénierie des Protéines, Département des Sciences de la Vie, Université de Liège, Sart Tilman, B4000 Liège, Belgium.
Bouhss A; Université Paris-Saclay, INSERM U1204, Univ Evry, Structure-Activité des Biomolécules Normales et Pathologiques (SABNP), F-91025 Evry-Courcouronnes, France.
Calvet-Vitale S; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.
Gravier-Pelletier C; Université de Paris, Faculté des Sciences, UMR CNRS 8601, LCBPT, F-75006 Paris, France.

Molecules ; 27(6)2022 Mar 08.

Article en En | MEDLINE | ID: mdl-35335131

RESUMEN

New inhibitors of the bacterial tranferase MraY are described. Their structure is based on an aminoribosyl uridine scaffold, which is known to be important for the biological activity of natural MraY inhibitors. A decyl alkyl chain was introduced onto this scaffold through various linkers. The synthesized compounds were tested against the MraYAA transferase activity, and the most active compound with an original (S,S)-tartaric diamide linker inhibits MraY activity with an IC50 equal to 0.37 µM. Their antibacterial activity was also evaluated on a panel of Gram-positive and Gram-negative strains; however, the compounds showed no antibacterial activity. Docking and molecular dynamics studies revealed that this new linker established two stabilizing key interactions with N190 and H325, as observed for the highly potent inhibitors carbacaprazamycin, muraymycin D2 and tunicamycin.

Asunto(s)

Diamida; Transferasas; Proteínas Bacterianas/química; Simulación de Dinámica Molecular; Transferasas/química; Transferasas (Grupos de Otros Fosfatos Sustitutos); Uridina/química; Uridina/farmacología

Palabras clave

MraY transferase; carbacaprazamycin analogs; inhibition tests; inhibitors synthesis; molecular docking studies

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Transferasas / Diamida Idioma: En Revista: Molecules Asunto de la revista: BIOLOGIA Año: 2022 Tipo del documento: Article País de afiliación: Francia

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