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Dive into the research topics where Dmytro Atamanyuk is active.

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Featured researches published by Dmytro Atamanyuk.


Journal of Medicinal Chemistry | 2013

Novel HldE-K inhibitors leading to attenuated Gram negative bacterial virulence.

Nicolas Desroy; Alexis Denis; Chrystelle Oliveira; Dmytro Atamanyuk; Sophia Briet; Fabien Faivre; Géraldine LeFralliec; Yannick Bonvin; Mayalen Oxoby; Sonia Escaich; Stéphanie Floquet; Elodie Drocourt; Vanida Vongsouthi; Lionel Durant; François Moreau; Theodore B. Verhey; Ting-Wai Lee; Murray S. Junop; Vincent Gerusz

We report here the optimization of an HldE kinase inhibitor to low nanomolar potency, which resulted in the identification of the first reported compounds active on selected E. coli strains. One of the most interesting candidates, compound 86, was shown to inhibit specifically bacterial LPS heptosylation on efflux pump deleted E. coli strains. This compound did not interfere with E. coli bacterial growth (MIC > 32 μg/mL) but sensitized this pathogen to hydrophobic antibiotics like macrolides normally inactive on Gram-negative bacteria. In addition, 86 could sensitize E. coli to serum complement killing. These results demonstrate that HldE kinase is a suitable target for drug discovery. They also pave the way toward novel possibilities of treating or preventing bloodstream infections caused by pathogenic Gram negative bacteria by inhibiting specific virulence factors.


Journal of Medicinal Chemistry | 2013

Structural-functional studies of Burkholderia cenocepacia D-glycero-β-D-manno-heptose 7-phosphate kinase (HldA) and characterization of inhibitors with antibiotic adjuvant and antivirulence properties.

Ting-Wai Lee; Theodore B. Verhey; Pavel A. Antiperovitch; Dmytro Atamanyuk; Nicolas Desroy; Chrystelle Oliveira; Alexis Denis; Vincent Gerusz; Elodie Drocourt; Mohamad A. Hamad; Christian Stanetty; Sara N. Andres; Seiji Sugiman-Marangos; Paul Kosma; Miguel A. Valvano; François Moreau; Murray S. Junop

As an essential constituent of the outer membrane of Gram-negative bacteria, lipopolysaccharide contributes significantly to virulence and antibiotic resistance. The lipopolysaccharide biosynthetic pathway therefore serves as a promising therapeutic target for antivirulence drugs and antibiotic adjuvants. Here we report the structural–functional studies of d-glycero-β-d-manno-heptose 7-phosphate kinase (HldA), an absolutely conserved enzyme in this pathway, from Burkholderia cenocepacia. HldA is structurally similar to members of the PfkB carbohydrate kinase family and appears to catalyze heptose phosphorylation via an in-line mechanism mediated mainly by a conserved aspartate, Asp270. Moreover, we report the structures of HldA in complex with two potent inhibitors in which both inhibitors adopt a folded conformation and occupy the nucleotide-binding sites. Together, these results provide important insight into the mechanism of HldA-catalyzed heptose phosphorylation and necessary information for further development of HldA inhibitors.


Journal of Medicinal Chemistry | 2013

Vectorization Efforts To Increase Gram-Negative Intracellular Drug Concentration: A Case Study on HldE-K Inhibitors

Dmytro Atamanyuk; Fabien Faivre; Mayalen Oxoby; Benoit Ledoussal; Elodie Drocourt; François Moreau; Vincent Gerusz

In this paper, we present different strategies to vectorize HldE kinase inhibitors with the goal to improve their gram-negative intracellular concentration. Syntheses and biological effects of siderophoric, aminoglycosidic, amphoteric, and polycationic vectors are discussed. While siderophoric and amphoteric vectorization efforts proved to be disappointing in this series, aminoglycosidic and polycationic vectors were able for the first time to achieve synergistic effects of our inhibitors with erythromycin. Although these effects proved to be nonspecific, this study provides information about the required stereoelectronic arrangement of the polycationic amines and their basicity requirements to fulfill outer membrane destabilization resulting in better erythromycin synergies.


Archive | 2012

Purine derivatives and their use as pharmaceuticals for prevention or treatment of bacterial infections

Dmytro Atamanyuk; Alexis Denis; Vincent Gerusz; Benoit Ledoussal; Yannick Bonvin; Nicolas Desroy; Johan Gold; François Moreau; Mayalen Oxoby


Archive | 2012

HEPTOSE DERIVATIVES FOR USE IN THE TREATMENT OF BACTERIAL INFECTIONS

Vincent Gerusz; Stéphane P. Vincent; Mayalen Oxoby; Dmytro Atamanyuk; François Moreau; Mounir Andaloussi; Abdellatif Tikad


Synthesis | 2017

Synthesis of 1,5-Anhydro-d-glycero-d-gluco-heptitol Derivatives as Potential Inhibitors of Bacterial Heptose Biosynthetic Pathways

Markus Blaukopf; Dmytro Atamanyuk; Nuno M. Xavier; Vincent Gerusz; Paul Kosma


Archive | 2015

New antibacterial compounds and biological applications thereof

Dmytro Atamanyuk; Vincent Gerusz; François Moreau; Vivien Henryon; Jérôme Monbrun; Etienne Airiau


Archive | 2015

Condensed derivatives of imidazole useful as pharmaceuticals

Dmytro Atamanyuk; Francis Chevreuil; Fabien Faivre; Nicolas Lecointe; Benoit Ledoussal; Chrystelle Oliveira; Christophe Simon


Archive | 2015

Heteroaromatic derivatives and their use as pharmaceuticals

Dmytro Atamanyuk; Francis Chevreuil; Fabien Faivre; Nicolas Lecointe; Benoit Ledoussal; Chrystelle Oliveira; Christophe Simon


Archive | 2015

3H-thieno[3,4]pyrimidin-4-one and pyrrolopyrimidone as gram-positive antibacterial agents

Dmytro Atamanyuk; Francis Chevreuil; Fabien Faivre; Vincent Gerusz; Johan Gold; François Moreau; Christophe Simon

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François Moreau

Centre national de la recherche scientifique

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François Moreau

Centre national de la recherche scientifique

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