Molecular Modelling and Atomistic Insights into the Binding Mechanism of MmpL3 Mtb

Samuel K Kwofie; George Hanson; Henrietta Sasu; Kweku S Enninful; Francis A Mensah; Richmond T Nortey; Omane P Yeboah; Clement Agoni; Michael D Wilson

doi:10.1002/cbdv.202200160

Molecular Modelling and Atomistic Insights into the Binding Mechanism of MmpL3 Mtb

Chem Biodivers. 2022 Sep;19(9):e202200160. doi: 10.1002/cbdv.202200160. Epub 2022 Aug 31.

Authors

Samuel K Kwofie^{1

2}, George Hanson^{1

3}, Henrietta Sasu^{1

3}, Kweku S Enninful³, Francis A Mensah¹, Richmond T Nortey¹, Omane P Yeboah¹, Clement Agoni^{4

5}, Michael D Wilson^{3

6}

Affiliations

¹ Department of Biomedical Engineering, School of Engineering Sciences, College of Basic & Applied Sciences, University of Ghana, PMB LG 77, Legon, 0000, Accra, Ghana.
² West African Center for Cell Biology of Infectious Pathogens, Department of Biochemistry, Cell and Molecular Biology, College of Basic and Applied Sciences, University of Ghana, 0000, Accra, Ghana.
³ Department of Parasitology, Noguchi Memorial Institute for Medical Research (NMIMR), College of Health Sciences (CHS), University of Ghana, P.O. Box LG 581, Legon, 0000, Accra, Ghana.
⁴ Conway Institute of Biomolecular and Biomedical Research, School of Medicine, University College of Dublin, Belfield, Dublin 4, Ireland.
⁵ Discipline of Pharmaceutical Sciences, University of KwaZulu Natal, X54001, Durban, South Africa.
⁶ Department of Medicine, Loyola University Medical Center, Maywood, IL, 60153, USA.

PMID: 35969844
DOI: 10.1002/cbdv.202200160

Abstract

Mycobacterial membrane proteins Large (MmpLs), which belong to the resistance, nodulation, and division (RND) protein superfamily, play critical roles in transporting polymers, lipids, and immunomodulators. MmpLs have become one of the important therapeutic drug targets to emerge in recent times. In this study, two homology modelling techniques, Modeller and SWISS-MODEL, were used in modelling the three-dimensional protein structure of the MmpL3 of Mycobacterium tuberculosis using that of M. smegmatis as template. MmpL3 inhibitors, namely BM212, NITD304, SPIRO, and NITD349, in addition to the co-crystalized ligands AU1235, ICA38, SQ109 and rimonabant, were screened against the modelled structure and the Mmpl3 of M. smegmatis using molecular docking techniques. Protein-ligand interactions were analysed using molecular dynamics simulations and Molecular Mechanics Poisson-Boltzmann surface area computations. Novel residues Gln32, Leu165, Ile414, and Phe35 were identified as critical for binding to M. tuberculosis MmpL3, and conformational dynamics upon inhibitor binding were discussed.

Keywords: Mycobacterium Smegmatis; Mycobacterium tuberculosis; molecular docking; molecular dynamics simulations; mycobacterial membrane proteins large (MmpL3).

MeSH terms

Antitubercular Agents / pharmacology
Bacterial Proteins / metabolism
Ligands
Membrane Proteins / metabolism
Membrane Transport Proteins
Molecular Docking Simulation
Mycobacterium tuberculosis*
Mycolic Acids* / metabolism
Polymers
Rimonabant / metabolism

Substances

Antitubercular Agents
Bacterial Proteins
Ligands
Membrane Proteins
Membrane Transport Proteins
Mycolic Acids
Polymers
Rimonabant

Grants and funding

West African Center for Cell Biology of Infectious Pathogens, University of Ghana