Abstract
The huge burden of leishmaniasis caused by the trypanosomatid protozoan parasite Leishmania is well known. This illness was included in the list of neglected tropical diseases targeted for elimination by the World Health Organization. However, the increasing evidence of resistance to existing antimonial drugs has made the eradication of the disease difficult to achieve, thus warranting the search for new drug targets. We report here studies that used computational methods to identify inhibitors of receptors from natural products. The cell division cycle-2-related kinase 12 (CRK12) receptor is a plausible drug target against Leishmania donovani. This study modelled the 3D molecular structure of the L. donovani CRK12 (LdCRK12) and screened for small molecules with potential inhibitory activity from African flora. An integrated library of 7722 African natural product-derived compounds and known inhibitors were screened against the LdCRK12 using AutoDock Vina after performing energy minimization with GROMACS 2018. Four natural products, namely sesamin (NANPDB1649), methyl ellagic acid (NANPDB1406), stylopine (NANPDB2581), and sennecicannabine (NANPDB6446) were found to be potential LdCRK12 inhibitory molecules. The molecular docking studies revealed two compounds NANPDB1406 and NANPDB2581 with binding affinities of −9.5 and −9.2 kcal/mol, respectively, against LdCRK12 which were higher than those of the known inhibitors and drugs, including GSK3186899, amphotericin B, miltefosine, and paromomycin. All the four compounds were predicted to have inhibitory constant (Ki) values ranging from 0.108 to 0.587 μM. NANPDB2581, NANPDB1649 and NANPDB1406 were also predicted as antileishmanial with Pa and Pi values of 0.415 and 0.043, 0.391 and 0.052, and 0.351 and 0.071, respectively. Molecular dynamics simulations coupled with molecular mechanics Poisson–Boltzmann surface area (MM/PBSA) computations reinforced their good binding mechanisms. Most compounds were observed to bind in the ATP binding pocket of the kinase domain. Lys488 was predicted as a key residue critical for ligand binding in the ATP binding pocket of the LdCRK12. The molecules were pharmacologically profiled as druglike with inconsequential toxicity. The identified molecules have scaffolds that could form the backbone for fragment-based drug design of novel leishmanicides but warrant further studies to evaluate their therapeutic potential.
Highlights
Leishmaniasis is a worldwide menace that exists in all continents except Oceania and it is endemic in the tropical and subtropical areas in Eastern Africa, Southern Europe, the Middle East, South-eastern Mexico, and Central and South America [1]
The selected hits were docked against the human cyclin-dependent kinase 9 (CDK9) since it is a homologue of the kinase domain of the L. donovani CRK12 (LdCRK12)
There was the need to model the structure of the LdCRK12 since there is no available structure in the protein data bank
Summary
Leishmaniasis is a worldwide menace that exists in all continents except Oceania and it is endemic in the tropical and subtropical areas in Eastern Africa, Southern Europe, the Middle East, South-eastern Mexico, and Central and South America [1]. One million new cases and between 26,000 to 65,000 deaths occur annually [2]. Leishmaniasis is a neglected tropical disease caused by the trypanosomatid protozoan Leishmania parasites transmitted to humans through the bites of infected phlebotomine sand flies [3,4,5,6,7]. Leishmaniasis has been observed with cases of co-infections in areas including the Mediterranean region, France, Italy, Portugal, Spain, Thailand, and Brazil [10,11,12]. VL co-infection with HIV-infected patients living in Asia (especially India) and some African countries have been reported [13]
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