Repurposing of <scp>FDA</scp>‐approved drugs as inhibitors of sterol C‐24 methyltransferase of <i>Leishmania donovani</i> to fight against leishmaniasis

Tabrez, Shams; Rahman, Farjana; Ali, Rahmat; Muhammad, Fida; Alshehri, Bader; Alaidarous, Mohammed; Banawas, Saeed; Dukhyil, Abdul Aziz Bin; Rub, Abdur

doi:10.1002/ddr.21820

Cited by 17 publications

(8 citation statements)

References 34 publications

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“…Though A1 , A2 , A3 , and A6 have similar core structures, they had different binding energies ( Table 2 ). Interestingly, using AutoDock Vina, compounds that had shown binding energies ≤−7.0 kcal/mol have been found to demonstrate significant inhibitory activities against the parasite of consideration ( Chang et al., 2007 ; Wyllie et al., 2018 ; Tabrez et al., 2021 ). In lieu of this, the predicted compounds may have the potential of suppressing Ld SMT since the binding energies were lower than −7.0 kcal/mol.…”

Section: Resultsmentioning

confidence: 99%

Homology Modeling, de Novo Design of Ligands, and Molecular Docking Identify Potential Inhibitors of Leishmania donovani 24-Sterol Methyltransferase

Sakyi

Broni

Amewu

et al. 2022

Front. Cell. Infect. Microbiol.

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The therapeutic challenges pertaining to leishmaniasis due to reported chemoresistance and toxicity necessitate the need to explore novel pathways to identify plausible inhibitory molecules. Leishmania donovani 24-sterol methyltransferase (LdSMT) is vital for the synthesis of ergosterols, the main constituents of Leishmania cellular membranes. So far, mammals have not been shown to possess SMT or ergosterols, making the pathway a prime candidate for drug discovery. The structural model of LdSMT was elucidated using homology modeling to identify potential novel 24-SMT inhibitors via virtual screening, scaffold hopping, and de-novo fragment-based design. Altogether, six potential novel inhibitors were identified with binding energies ranging from −7.0 to −8.4 kcal/mol with e-LEA3D using 22,26-azasterol and S1–S4 obtained from scaffold hopping via the ChEMBL, DrugBank, PubChem, ChemSpider, and ZINC15 databases. These ligands showed comparable binding energy to 22,26-azasterol (−7.6 kcal/mol), the main inhibitor of LdSMT. Moreover, all the compounds had plausible ligand efficiency-dependent lipophilicity (LELP) scores above 3. The binding mechanism identified Tyr92 to be critical for binding, and this was corroborated via molecular dynamics simulations and molecular mechanics Poisson–Boltzmann surface area (MM-PBSA) calculations. The ligand A1 was predicted to possess antileishmanial properties with a probability of activity (Pa) of 0.362 and a probability of inactivity (Pi) of 0.066, while A5 and A6 possessed dermatological properties with Pa values of 0.205 and 0.249 and Pi values of 0.162 and 0.120, respectively. Structural similarity search via DrugBank identified vabicaserin, daledalin, zanapezil, imipramine, and cefradine with antileishmanial properties suggesting that the de-novo compounds could be explored as potential antileishmanial agents.

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Section: Resultsmentioning

confidence: 99%

Homology Modeling, de Novo Design of Ligands, and Molecular Docking Identify Potential Inhibitors of Leishmania donovani 24-Sterol Methyltransferase

Sakyi

Broni

Amewu

et al. 2022

Front. Cell. Infect. Microbiol.

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“…Molecular docking has been explored in the identification of lead compounds including gentisic acid 5-O glucoside [ 59 ], simeprevir [ 28 ], and bisindolylmaleimide IX [ 74 ] by targeting Buruli ulcer [ 59 ], visceral leishmaniasis [ 28 ], and SARS-CoV-2 [ 74 ], respectively. In all these instances, the binding energies associated with the protein–ligand complexes were used as part of the criteria to shortlist the hits.…”

Section: Resultsmentioning

confidence: 99%

“…To improve the inhibitory effect of 22,26-azsterol, some analogues ( Figure 1 ) were generated, and their activities were found to be dependent on the presence of ammonium or sulfonium functionality in the side chain [ 25 ]. Similarly, ezetimibe, imipramine, and simeprevir ( Figure 1 ) have shown promising inhibitory activity against L. donovani by making morphological changes to the plasma and mitochondrion membranes with IC 50 of 30, 28.6, and 51.49 μM, respectively [ 26 , 27 , 28 ]. A fragment-based de novo design was used to predict potential inhibitors against L. donovani sterol methyltransferase ( Ld SMT) [ 29 ].…”

Section: Introductionmentioning

confidence: 99%

Inhibiting Leishmania donovani Sterol Methyltransferase to Identify Lead Compounds Using Molecular Modelling

et al. 2023

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The recent outlook of leishmaniasis as a global public health concern coupled with the reportage of resistance and lack of efficacy of most antileishmanial drugs calls for a concerted effort to find new leads. The study combined In silico and in vitro approaches to identify novel potential synthetic small-molecule inhibitors targeting the Leishmania donovani sterol methyltransferase (LdSMT). The LdSMT enzyme in the ergosterol biosynthetic pathway is required for the parasite’s membrane fluidity, distribution of membrane proteins, and control of the cell cycle. The lack of LdSMT homologue in the human host and its conserved nature among all Leishmania parasites makes it a viable target for future antileishmanial drugs. Initially, six known inhibitors of LdSMT with IC50 < 10 μM were used to generate a pharmacophore model with a score of 0.9144 using LigandScout. The validated model was used to screen a synthetic library of 95,630 compounds obtained from InterBioScreen limited. Twenty compounds with pharmacophore fit scores above 50 were docked against the modelled three-dimensional structure of LdSMT using AutoDock Vina. Consequently, nine compounds with binding energies ranging from −7.5 to −8.7 kcal/mol were identified as potential hit molecules. Three compounds comprising STOCK6S-06707, STOCK6S-84928, and STOCK6S-65920 with respective binding energies of −8.7, −8.2, and −8.0 kcal/mol, lower than 22,26-azasterol (−7.6 kcal/mol), a known LdSMT inhibitor, were selected as plausible lead molecules. Molecular dynamics simulation studies and molecular mechanics Poisson–Boltzmann surface area calculations showed that the residues Asp25 and Trp208 were critical for ligand binding. The compounds were also predicted to have antileishmanial activity with reasonable pharmacological and toxicity profiles. When the antileishmanial activity of the three hits was evaluated in vitro against the promastigotes of L. donovani, mean half-maximal inhibitory concentrations (IC50) of 21.9 ± 1.5 μM (STOCK6S-06707), 23.5 ± 1.1 μM (STOCK6S-84928), and 118.3 ± 5.8 μM (STOCK6S-65920) were obtained. Furthermore, STOCK6S-84928 and STOCK6S-65920 inhibited the growth of Trypanosoma brucei, with IC50 of 14.3 ± 2.0 μM and 18.1 ± 1.4 μM, respectively. The identified compounds could be optimised to develop potent antileishmanial therapeutic agents.

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“…Although medicine donation programs are multiplying to support the burden of neglected tropical diseases [150] such as leishmaniases, the pharmaceutical industry seems to increasingly restrict its research and development investment to new drug candidates [151]. Alternative options consist of repurposing drugs [152][153][154] or improving existing drugs, such as the gold standard amphotericin B [155]. Nevertheless, research into new drug candidates that are active against Leishmania must not be excluded, especially as methodological tools are becoming increasingly effective.…”

Section: Discussionmentioning

confidence: 99%

Challenges and Tools for In Vitro Leishmania Exploratory Screening in the Drug Development Process: An Updated Review

Cohen

Azas

2021

Pathogens

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Leishmaniases are a group of vector-borne diseases caused by infection with the protozoan parasites Leishmania spp. Some of them, such as Mediterranean visceral leishmaniasis, are zoonotic diseases transmitted from vertebrate to vertebrate by a hematophagous insect, the sand fly. As there is an endemic in more than 90 countries worldwide, this complex and major health problem has different clinical forms depending on the parasite species involved, with the visceral form being the most worrying since it is fatal when left untreated. Nevertheless, currently available antileishmanial therapies are significantly limited (low efficacy, toxicity, adverse side effects, drug-resistance, length of treatment, and cost), so there is an urgent need to discover new compounds with antileishmanial activity, which are ideally inexpensive and orally administrable with few side effects and a novel mechanism of action. Therefore, various powerful approaches were recently applied in many interesting antileishmanial drug development programs. The objective of this review is to focus on the very first step in developing a potential drug and to identify the exploratory methods currently used to screen in vitro hit compounds and the challenges involved, particularly in terms of harmonizing the results of work carried out by different research teams. This review also aims to identify innovative screening tools and methods for more extensive use in the drug development process.

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Repurposing of FDA‐approved drugs as inhibitors of sterol C‐24 methyltransferase of Leishmania donovani to fight against leishmaniasis

Cited by 17 publications

References 34 publications

Homology Modeling, de Novo Design of Ligands, and Molecular Docking Identify Potential Inhibitors of Leishmania donovani 24-Sterol Methyltransferase

Homology Modeling, de Novo Design of Ligands, and Molecular Docking Identify Potential Inhibitors of Leishmania donovani 24-Sterol Methyltransferase

Inhibiting Leishmania donovani Sterol Methyltransferase to Identify Lead Compounds Using Molecular Modelling

Challenges and Tools for In Vitro Leishmania Exploratory Screening in the Drug Development Process: An Updated Review

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