4.5 Article

Mce1R of Mycobacterium tuberculosis prefers long-chain fatty acids as specific ligands: a computational study

Journal

MOLECULAR DIVERSITY
Volume 27, Issue 6, Pages 2523-2543

Publisher

SPRINGER
DOI: 10.1007/s11030-022-10566-7

Keywords

Rv0165c; Mce1R; VanR family; Molecular docking; Protein-ligand interaction; MD simulation

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Mce1R, a VanR-type regulator, transcriptionally regulates the mce1 operon of Mycobacterium tuberculosis by binding specific ligands. This study computationally identified Mce1R-specific ligands and found that it preferably binds to long-chain fatty acids, leading to distinct structural changes.
The mce1 operon of Mycobacterium tuberculosis, which codes the Mce1 transporter, facilitates the transport of fatty acids. Fatty acids are one of the major sources for carbon and energy for the pathogen during its intracellular survival and pathogenicity. The mce1 operon is transcriptionally regulated by Mce1R, a VanR-type regulator, which could bind specific ligands and control the expression of the mce1 operon accordingly. This work reports computational identification of Mce1R-specific ligands. Initially by employing cavity similarity search algorithm by the ProBis server, the cavities of the proteins similar to that of Mce1R and the bound ligands were identified from which fatty acids were selected as the potential ligands. From the earlier-generated monomeric structure, the dimeric structure of Mce1R was then modeled by the GalaxyHomomer server and validated computationally to use in molecular docking and molecular dynamics simulation analysis. The fatty acid ligands were found to dock within the cavity of Mce1R and the docked complexes were subjected to molecular dynamics simulation to explore their stabilities and other dynamic properties. The data suggest that Mce1R preferably binds to long-chain fatty acids and undergoes distinct structural changes upon binding.

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