Antileishmanial Drug Discovery and Development: Time to Reset the Model?

Olías-Molero, Ana Isabel; Fuente, Concepción de la; Cuquerella, Montserrat; Torrado, J. J.; Alunda, José María

doi:10.3390/microorganisms9122500

Cited by 38 publications

(42 citation statements)

References 178 publications

(225 reference statements)

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“…The range of currently available drugs for treating leishmaniasis is relatively small and it includes notably 62.5% of repurposed molecules, while less than 1% of all new drug candidates reached clinical trials in the last decades [42,43]. For these reasons, the investigation of new therapies has been very active recently, whereas a wide range of compounds has been identified as potential hits and leads [44].…”

Section: Discussionmentioning

confidence: 99%

In silico-based screening for natural product’s structural analogs as new drugs candidate against leishmaniasis

Barazorda-Ccahuana

Goyzueta-Mamani

Candia-Puma

et al. 2022

Preprint

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Leishmaniasis is a disease with high mortality rates and approximately 1.5 million new cases each year. Despite the new approaches and advances to fight the disease, there are no effective therapies. Hence, this study aims to in silico screen for natural product's structural analogs as new drugs candidate against leishmaniasis. We applied in silico analysis, such as virtual screening, molecular docking, molecular dynamics simulation, and Molecular Mechanics-Generalized Born Surface Area MM/GBSA estimation aiming to select structural analogs from natural products that have shown antileishmanial activity against arginase (ARG) enzyme and that could bind selectively against Leishmania ARG. The compounds 2H-1-Benzopyran, 3,4-dihydro-2-(2-methylphenyl)- (9CI), Echioidinin, and Malvidin showed good results against ARG targets from three parasite species and negative results for potential toxicities. The Malvidin ligand generated interactions in the active center at pH 2.0 conditions and hydrogen bonds enhancing receptor-ligand coupling. This work identified Malvidin as a potential drug candidate to treat leishmaniasis.

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Section: Discussionmentioning

confidence: 99%

In silico-based screening for natural product’s structural analogs as new drugs candidate against leishmaniasis

Barazorda-Ccahuana

Goyzueta-Mamani

Candia-Puma

et al. 2022

Preprint

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“…Despite considerable progress in the understanding of the molecular biology of Leishmania sp., antileishmanial chemotherapy remains limited to a few chemical series. Thus, for the last 70 years, pentavalent antimony compounds such as sodium stibogluconate (Pentostam ® , GSK) and meglumine antimoniate (Glucantime ® , Sanofi) have been the first-line treatment for leishmaniases [ 4 ]. Parenteral alternatives to antimonials such as liposomal amphotericin B (AmBisome ® , Gilead) have fewer side effects, while miltefosine (Impavido ® , Zentaris) was the first orally active antileishmanial drug to be developed.…”

Section: Introductionmentioning

confidence: 99%

“…Parenteral alternatives to antimonials such as liposomal amphotericin B (AmBisome ® , Gilead) have fewer side effects, while miltefosine (Impavido ® , Zentaris) was the first orally active antileishmanial drug to be developed. Paromomycin can also be used, but resistance is developing rapidly, meaning that it is used only in drug combinations [ 4 ]. These currently used drugs are presented in Figure 1 .…”

Section: Introductionmentioning

confidence: 99%

The Potential of 2-Substituted Quinolines as Antileishmanial Drug Candidates

et al. 2022

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There is a need for new, cost-effective drugs to treat leishmaniasis. A strategy based on traditional medicine practiced in Bolivia led to the discovery of the 2-substituted quinoline series as a source of molecules with antileishmanial activity and low toxicity. This review documents the development of the series from the first isolated natural compounds through several hundred synthetized molecules to an optimized compound exhibiting an in vitro IC50 value of 0.2 µM against Leishmania donovani, and a selectivity index value of 187, together with in vivo activity on the L. donovani/hamster model. Attempts to establish structure–activity relationships are described, as well as studies that have attempted to determine the mechanism of action. For the latter, it appears that molecules of this series act on multiple targets, possibly including the immune system, which could explain the observed lack of drug resistance after in vitro drug pressure. We also show how nanotechnology strategies could valorize these drugs through adapted formulations and how a mechanistic targeting approach could generate new compounds with increased activity.

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“…It is clearly important for long-term health and well-being to populate the pipeline of new medicines to treat VL, CL and PKDL. The emergence of strains resistant to even the most recently introduced drugs such as miltefosine is critical, and a lack of investment in this neglected tropical disease means that there are few new drugs being developed [ 7 ].…”

Section: Introductionmentioning

confidence: 99%

Selective Anti-Leishmanial Strathclyde Minor Groove Binders Using an N-Oxide Tail-Group Modification

Perieteanu

McGee²,

Shaw³

et al. 2022

IJMS

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The neglected tropical disease leishmaniasis, caused by Leishmania spp., is becoming more problematic due to the emergence of drug-resistant strains. Therefore, new drugs to treat leishmaniasis, with novel mechanisms of action, are urgently required. Strathclyde minor groove binders (S-MGBs) are an emerging class of anti-infective agent that have been shown to have potent activity against various bacteria, viruses, fungi and parasites. Herein, it is shown that S-MGBs have potent activity against L. donovani, and that an N-oxide derivation of the tertiary amine tail of typical S-MGBs leads to selective anti-leishmanial activity. Additionally, using S-MGB-219, the N-oxide derivation is shown to retain strong binding to DNA as a 2:1 dimer. These findings support the further study of anti-leishmanial S-MGBs as novel therapeutics.

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Antileishmanial Drug Discovery and Development: Time to Reset the Model?

Cited by 38 publications

References 178 publications

In silico-based screening for natural product’s structural analogs as new drugs candidate against leishmaniasis

In silico-based screening for natural product’s structural analogs as new drugs candidate against leishmaniasis

The Potential of 2-Substituted Quinolines as Antileishmanial Drug Candidates

Selective Anti-Leishmanial Strathclyde Minor Groove Binders Using an N-Oxide Tail-Group Modification

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