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

Cohen, Anita; Azas, Nadine

doi:10.3390/pathogens10121608

Cited by 9 publications

(11 citation statements)

References 147 publications

(152 reference statements)

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“…One of the major bottlenecks in drug discovery is the identification of the molecular targets of a compound ( Fernández-Prada et al., 2019 ; Cohen and Azas, 2021 ), which, if not fully elucidated, hinders subsequent structure-activity relationship studies that have the potential to contribute to drug optimization and drug development ( Terstappen et al., 2007 ). While proteomic-based approaches have become a cornerstone in the study of MoA and MoDR in Leishmania parasites, there remain important knowledge gaps to fill before these mechanisms are holistically understood ( Fernandez-Prada et al., 2018b ; Bhattacharya et al., 2020 ; Douanne et al., 2020a ).…”

Section: Discussionmentioning

confidence: 99%

Exploring direct and indirect targets of current antileishmanial drugs using a novel thermal proteomics profiling approach

Ibarra-Meneses

Corbeil²,

Wagner³

et al. 2022

Front. Cell. Infect. Microbiol.

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Visceral leishmaniasis (VL), caused by Leishmania infantum, is an oft-fatal neglected tropical disease. In the absence of an effective vaccine, the control of leishmaniasis relies exclusively on chemotherapy. Due to the lack of established molecular/genetic markers denoting parasite resistance, clinical treatment failure is often used as an indicator. Antimony-based drugs have been the standard antileishmanial treatment for more than seven decades, leading to major drug resistance in certain regions. Likewise, drug resistance to miltefosine and amphotericin B continues to spread at alarming rates. In consequence, innovative approaches are needed to accelerate the identification of antimicrobial drug targets and resistance mechanisms. To this end, we have implemented a novel approach based on thermal proteome profiling (TPP) to further characterize the mode of action of antileishmanials antimony, miltefosine and amphotericin B, as well as to better understand the mechanisms of drug resistance deployed by Leishmania. Proteins become more resistant to heat-induced denaturation when complexed with a ligand. In this way, we used multiplexed quantitative mass spectrometry-based proteomics to monitor the melting profile of thousands of expressed soluble proteins in WT, antimony-resistant, miltefosine-resistant, and amphotericin B-resistant L. infantum parasites, in the presence (or absence) of the above-mentioned drugs. Bioinformatics analyses were performed, including data normalization, melting profile fitting, and identification of proteins that underwent changes (fold change > 4) caused by complexation with a drug. With this unique approach, we were able to narrow down the regions of the L. infantum proteome that interact with antimony, miltefosine, and amphotericin B; validating previously-identified and unveiling novel drug targets. Moreover, analyses revealed candidate proteins potentially involved in drug resistance. Interestingly, we detected thermal proximity coaggregation for several proteins belonging to the same metabolic pathway (i.e., tryparedoxin peroxidase and aspartate aminotransferase in proteins exposed to antimony), highlighting the importance of these pathways. Collectively, our results could serve as a jumping-off point for the future development of innovative diagnostic tools for the detection and evaluation of antimicrobial-resistant Leishmania populations, as well as open the door for new on-target therapies.

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Section: Discussionmentioning

confidence: 99%

Exploring direct and indirect targets of current antileishmanial drugs using a novel thermal proteomics profiling approach

Ibarra-Meneses

Corbeil²,

Wagner³

et al. 2022

Front. Cell. Infect. Microbiol.

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“…Bioluminescent reporter lines of Leishmania spp. have been used to monitor parasite viability in the context of drug and vaccine screening ( Caridha et al., 2017 ; Álvarez-Velilla et al., 2019 ; Mendes Costa et al., 2019 ; Agostino et al., 2020 ; Cohen and Azas, 2021 ), but to our knowledge, not within the context of ‘omics’ screens.…”

Section: Imagingmentioning

confidence: 99%

Paving the Way: Contributions of Big Data to Apicomplexan and Kinetoplastid Research

Kent

Briggs²,

Colon³

et al. 2022

Front. Cell. Infect. Microbiol.

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In the age of big data an important question is how to ensure we make the most out of the resources we generate. In this review, we discuss the major methods used in Apicomplexan and Kinetoplastid research to produce big datasets and advance our understanding of Plasmodium, Toxoplasma, Cryptosporidium, Trypanosoma and Leishmania biology. We debate the benefits and limitations of the current technologies, and propose future advancements that may be key to improving our use of these techniques. Finally, we consider the difficulties the field faces when trying to make the most of the abundance of data that has already been, and will continue to be, generated.

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“…The Leishmania lifecycle requires the presence of a sand fly vector and a mammalian host that causes the existence of two distinct morphological forms (promastigote and amastigote). Although the amastigote form is found in host cells and is considered the target form of the parasite, its determination of IC50 consists of a time-consuming and laborious procedure and is not suitable for a large-scale screening method [54]. In general, exploratory screening methods designed to accelerate the testing of many compounds are performed on the promastigote form [54,55].…”

Section: Antipromastigote Assay and Cytotoxicity Elucidationmentioning

confidence: 99%

Flavonoid Derivatives as New Potent Inhibitors of Cysteine Proteases: An Important Step toward the Design of New Compounds for the Treatment of Leishmaniasis

Lourenço¹,

Iório²,

Silva³

et al. 2022

Preprint

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Leishmaniasis is a neglected tropical disease and affects more than 350 million people worldwide. However, there are no vaccines for humans, and current treatment is hampered due to its high cost, numerous side effects, and painful administration routes. Ending its epidemics by 2030 has become a United Nations goal, and the multitarget drug strategy emerges as a promising alternative. Flavonoids are an example of multitarget compounds and organic synthesis represents a tool to obtain high yields of these molecules. In our study, we synthesized 17 flavonoid analogs using a scalable, easy-to-reproduce, and inexpensive method. All compounds demonstrated an impressive inhibition capacity against rCPB2.8, rCPB3, and rH84Y, which are highly expressed in the amastigote stage, the target form of the parasite. Compounds 3c, f12a, and f12b stood out as effective against all isoforms and intermolecular interactions were investigated through a molecular modeling study. The compounds were highly potent against the parasite and demonstrated low cytotoxic action against mammalian cells. The results were pioneering, representing an advance in the investigation of the mechanisms behind the antileishmanial action of flavonoid derivatives. Furthermore, compounds have shown to be promising leads for the design of other cysteine protease inhibitors for the treatment of leishmaniasis diseases.

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

Cited by 9 publications

References 147 publications

Exploring direct and indirect targets of current antileishmanial drugs using a novel thermal proteomics profiling approach

Exploring direct and indirect targets of current antileishmanial drugs using a novel thermal proteomics profiling approach

Paving the Way: Contributions of Big Data to Apicomplexan and Kinetoplastid Research

Flavonoid Derivatives as New Potent Inhibitors of Cysteine Proteases: An Important Step toward the Design of New Compounds for the Treatment of Leishmaniasis

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