Broad-spectrum in vitro activity of macrophage infectivity potentiator inhibitors against Gram-negative bacteria and Leishmania major

Author:

Iwasaki Jua123,Lorimer Donald D.45,Vivoli-Vega Mirella67,Kibble Emily A.189,Peacock Christopher S.1,Abendroth Jan45,Mayclin Stephen J.45,Dranow David M.45,Pierce Phillip G.45,Fox David45,Lewis Maria1,Bzdyl Nicole M.1,Kristensen Sofie S.1,Inglis Timothy J. J.1011,Kahler Charlene M.1,Bond Charles S.12ORCID,Hasenkopf Anja13,Seufert Florian13,Schmitz Jens13,Marshall Laura E.14,Scott Andrew E.14,Norville Isobel H.14,Myler Peter J.4,Holzgrabe Ulrike13,Harmer Nicholas J.67ORCID,Sarkar-Tyson Mitali1

Affiliation:

1. Marshall Centre for Infectious Disease Research and Training, School of Biomedical Sciences, The University of Western Australia , Perth, Western Australia, 6008, Australia

2. Wesfarmers Centre for Vaccines and Infectious Diseases, Telethon Kids Institute, University of Western Australia , Nedlands, Western Australia, 6008, Australia

3. Centre for Child Health Research, University of Western Australia , Perth, Western Australia, 6008, Australia

4. Seattle Structural Genomics Center for Infectious Disease , 307 Westlake Avenue North, Seattle, WA, 98109, USA

5. Beryllium, Inc. , 7869 NE Day Road West, Bainbridge Island, WA 98110, USA

6. Department of Biosciences , Geoffrey Pope Building, Stocker Road, Exeter, EX4 4QD, UK

7. Living Systems Institute , Stocker Road, Exeter, EX4 4QD, UK

8. School of Veterinary and Life Sciences, Murdoch University , Perth, WA, Australia

9. DMTC Limited, Level 2 , 24 Wakefield St, Hawthorn, VIC 3122, Australia

10. Department of Microbiology, PathWest Laboratory Medicine , Nedlands, WA 6009, Australia

11. Medical School, University of Western Australia , Nedlands, WA 6009, Australia

12. School of Molecular Sciences, The University of Western Australia , Perth, Western Australia, 6009, Australia

13. Institute of Pharmacy and Food Chemistry, University of Würzburg , Am Hubland, 97074 Würzburg, Germany

14. Defence Science and Technology Laboratory, Porton Down , Salisbury, UK

Abstract

Abstract Background The macrophage infectivity potentiator (Mip) protein, which belongs to the immunophilin superfamily, is a peptidyl-prolyl cis/trans isomerase (PPIase) enzyme. Mip has been shown to be important for virulence in a wide range of pathogenic microorganisms. It has previously been demonstrated that small-molecule compounds designed to target Mip from the Gram-negative bacterium Burkholderia pseudomallei bind at the site of enzymatic activity of the protein, inhibiting the in vitro activity of Mip. Objectives In this study, co-crystallography experiments with recombinant B. pseudomallei Mip (BpMip) protein and Mip inhibitors, biochemical analysis and computational modelling were used to predict the efficacy of lead compounds for broad-spectrum activity against other pathogens. Methods Binding activity of three lead compounds targeting BpMip was verified using surface plasmon resonance spectroscopy. The determination of crystal structures of BpMip in complex with these compounds, together with molecular modelling and in vitro assays, was used to determine whether the compounds have broad-spectrum antimicrobial activity against pathogens. Results Of the three lead small-molecule compounds, two were effective in inhibiting the PPIase activity of Mip proteins from Neisseria meningitidis, Klebsiella pneumoniae and Leishmania major. The compounds also reduced the intracellular burden of these pathogens using in vitro cell infection assays. Conclusions These results indicate that Mip is a novel antivirulence target that can be inhibited using small-molecule compounds that prove to be promising broad-spectrum drug candidates in vitro. Further optimization of compounds is required for in vivo evaluation and future clinical applications.

Funder

SSGCID

NIAID

NIH

NATO

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology,Microbiology (medical)

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