Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Reader, Janette; Watt, Mariëtte van der; Taylor, Dale; Manach, Claire Le; Mittal, Nimisha; Ottilie, Sabine; Theron, Anjo; Moyo, Phanankosi; Erlank, Erica; Nardini, Luisa; Venter, Nelius; Lauterbach, Sonja; Bezuidenhout, Belinda; Horatscheck, André; Heerden, Ashleigh van; Spillman, Natalie J.; Cowell, Anne N.; Connacher, Jessica; Opperman, D.P.J.; Orchard, Lindsey M.; Llinás, Manuel; Istvan, Eva S.; Goldberg, Daniel E.; Boyle, Grant A.; Calvo, David; Mancama, D; Coetzer, Thérèsa L.; Winzeler, Elizabeth A.; Duffy, James; Koekemoer, Lizette L.; Basarab, Gregory S.; Chibale, Kelly; Birkholtz, Lyn Marié

doi:10.1038/s41467-020-20629-8

Cited by 72 publications

(108 citation statements)

References 79 publications

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“…Asexual blood stage parasites treated with compounds with different MoAs show distinct and divergent transcriptomic responses ( Hu et al., 2009 ; Siwo et al., 2015 ; van der Watt et al., 2018 ). This has also been observed for immature gametocytes ( Ngwa et al., 2017 ; Ngwa et al., 2019 ; Reader et al., 2021 ), which implies that chemically-induced transcriptome responses can be detected for various life cycle stages of the parasite. The parasite’s transcriptome can therefore be mined to stratify compounds to specific MoAs.…”

Section: Introductionmentioning

confidence: 66%

“…Additionally, such compounds should have a novel mode of action (MoA) and will be used in combination with each other to lower the rate of resistance emergence ( Verlinden et al., 2016 ). Phenotypic whole-cell screening has successfully delivered thousands of hit compounds [validated hits ( Quancard et al., 2021 )] with nanomolar whole-cell activity against multiple life cycle stages of P. falciparum ( Plouffe et al., 2008 ; Gamo et al., 2010 ; Delves, 2012 ; Miguel-Blanco et al., 2017 ; Delves et al., 2018 ; Delves et al., 2019 ; Abraham et al., 2020 ; Reader et al., 2021 ). However, this process is not guided by any knowledge on a compounds’ MoA or target.…”

Section: Introductionmentioning

confidence: 99%

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Machine Learning Uses Chemo-Transcriptomic Profiles to Stratify Antimalarial Compounds With Similar Mode of Action

Heerden

Wyk

Birkholtz

2021

Front. Cell. Infect. Microbiol.

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The rapid development of antimalarial resistance motivates the continued search for novel compounds with a mode of action (MoA) different to current antimalarials. Phenotypic screening has delivered thousands of promising hit compounds without prior knowledge of the compounds’ exact target or MoA. Whilst the latter is not initially required to progress a compound in a medicinal chemistry program, identifying the MoA early can accelerate hit prioritization, hit-to-lead optimization and preclinical combination studies in malaria research. The effects of drug treatment on a cell can be observed on systems level in changes in the transcriptome, proteome and metabolome. Machine learning (ML) algorithms are powerful tools able to deconvolute such complex chemically-induced transcriptional signatures to identify pathways on which a compound act and in this manner provide an indication of the MoA of a compound. In this study, we assessed different ML approaches for their ability to stratify antimalarial compounds based on varied chemically-induced transcriptional responses. We developed a rational gene selection approach that could identify predictive features for MoA to train and generate ML models. The best performing model could stratify compounds with similar MoA with a classification accuracy of 76.6 ± 6.4%. Moreover, only a limited set of 50 biomarkers was required to stratify compounds with similar MoA and define chemo-transcriptomic fingerprints for each compound. These fingerprints were unique for each compound and compounds with similar targets/MoA clustered together. The ML model was specific and sensitive enough to group new compounds into MoAs associated with their predicted target and was robust enough to be extended to also generate chemo-transcriptomic fingerprints for additional life cycle stages like immature gametocytes. This work therefore contributes a new strategy to rapidly, specifically and sensitively indicate the MoA of compounds based on chemo-transcriptomic fingerprints and holds promise to accelerate antimalarial drug discovery programs.

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Section: Introductionmentioning

confidence: 66%

Section: Introductionmentioning

confidence: 99%

Machine Learning Uses Chemo-Transcriptomic Profiles to Stratify Antimalarial Compounds With Similar Mode of Action

Heerden

Wyk

Birkholtz

2021

Front. Cell. Infect. Microbiol.

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“…In these organisms, one of the suggested mechanisms is again that the compound acts as a protonophore uncoupler and rapidly collapses the mitochondrial membrane potential [9][10][11]. In addition, as with the kinetoplastid parasites, SQ109 was also found to have potent in vitro activity against Plasmodium falciparum where it was shown to selectively inhibit mature gametocytes (stage IV/V), the stage responsible for transmission, with an IC50 value of 0.105 µM [13]. With the generation of an SQ109-resistant clone, mutations in One such example is the anti-tubercular drug candidate SQ109 [N-adamantan-2-yl-N'-((E)-3,7-dimethyl-octa-2,6-dienyl)-ethane-1,2-diamine] which has been found have potent activity against kinetoplastid parasites in vitro [7][8][9][10][11], but there have been no reports of its activity in vivo in any protozoa.…”

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

In Vivo Efficacy of SQ109 against Leishmania donovani, Trypanosoma spp. and Toxoplasma gondii and In Vitro Activity of SQ109 Metabolites

et al. 2022

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SQ109 is an anti-tubercular drug candidate that has completed Phase IIb/III clinical trials for tuberculosis and has also been shown to exhibit potent in vitro efficacy against protozoan parasites including Leishmania and Trypanosoma cruzi spp. However, its in vivo efficacy against protozoa has not been reported. Here, we evaluated the activity of SQ109 in mouse models of Leishmania, Trypanosoma spp. as well as Toxoplasma infection. In the T. cruzi mouse model, 80% of SQ109-treated mice survived at 40 days post-infection. Even though SQ109 did not cure all mice, these results are of interest since they provide a basis for future testing of combination therapies with the azole posaconazole, which acts synergistically with SQ109 in vitro. We also found that SQ109 inhibited the growth of Toxoplasma gondii in vitro with an IC50 of 1.82 µM and there was an 80% survival in mice treated with SQ109, whereas all untreated animals died 10 days post-infection. Results with Trypanosoma brucei and Leishmania donovani infected mice were not promising with only moderate efficacy. Since SQ109 is known to be extensively metabolized in animals, we investigated the activity in vitro of SQ109 metabolites. Among 16 metabolites, six mono-oxygenated forms were found active across the tested protozoan parasites, and there was a ~6× average decrease in activity of the metabolites as compared to SQ109 which is smaller than the ~25× found with mycobacteria.

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“…Pillar 2 of this strategy is to accelerate efforts toward the elimination of malaria and attainment of malaria-free status. All evidence shows the fact that malaria elimination will require new strategies not only to target the hepatic stage, the erythrocytic stage, and the gametocyte development stages to prevent transmission to vectors but also to target the sporogonic stages inside the vector to prevent transmission to a new human host ( 2 , 9 , 10 ). The hepatic and sporogonic stages of the malaria parasite have remained largely underexploited as antimalarial targets, due to the poorly understood biology of these life cycle stages and the inherent technical difficulties in studying them ( 10 , 11 ).…”

Section: Introductionmentioning

confidence: 99%

A New Thienopyrimidinone Chemotype Shows Multistage Activity against Plasmodium falciparum, Including Artemisinin-Resistant Parasites

et al. 2021

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This work reports a new chemical structure that (i) displays activity against the human malaria parasite Plasmodium falciparum at 3 stages of the parasitic cycle (blood stage, hepatic stage, and sexual stages), (ii) remains active against parasites that are resistant to the first-line treatment recommended by the World Health Organization (WHO) for the treatment of severe malaria (artemisinins), and (iii) reduces transmission of the parasite to the mosquito vector in a mouse model. This new molecule family could open the way to the conception of novel antimalarial drugs with an original multistage mechanism of action to fight against Plasmodium drug resistance and block interhuman transmission of malaria.

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Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Cited by 72 publications

References 79 publications

Machine Learning Uses Chemo-Transcriptomic Profiles to Stratify Antimalarial Compounds With Similar Mode of Action

Machine Learning Uses Chemo-Transcriptomic Profiles to Stratify Antimalarial Compounds With Similar Mode of Action

In Vivo Efficacy of SQ109 against Leishmania donovani, Trypanosoma spp. and Toxoplasma gondii and In Vitro Activity of SQ109 Metabolites

A New Thienopyrimidinone Chemotype Shows Multistage Activity against Plasmodium falciparum, Including Artemisinin-Resistant Parasites

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