A novel in vitro image-based assay identifies new drug leads for giardiasis

Hart, Christopher J; Munro, Taylah; Andrews, Katherine Thea; Ryan, John H.; Riches, Andrew G.; Skinner‐Adams, Tina S.

doi:10.1016/j.ijpddr.2017.01.005

Cited by 21 publications

(29 citation statements)

References 51 publications

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“… 79 The efficacy of Malaria Box, a collection of 400 diverse compounds with antimalarial activity, as well as an other 1,600 known bioactive molecules, has been tested using an automated live-cell digital phase-contrast microscopy assay that permits automated assessment of Giardia growth without cell staining. 81 , 82 Other assays instead rely on transgenic Giardia parasites, based on either the assessment of glucuronidase activity in trophozoites 83 or the amount of luciferase bioluminescence in trophozoites and encysting parasites, the latest allowing bioluminescent monitoring of the drug efficacy in mouse infection model by imaging methods. 84 This last option is of paramount importance, since the increasing use of murine model of giardiasis is required for the pre-clinical evaluation of undesired pharmacokinetic/ pharmacodynamic properties.…”

Section: Introductionmentioning

confidence: 99%

Treatment-refractory giardiasis: challenges and solutions

Lalle

Hanevik

2018

IDR

108

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Giardia is the commonest parasitic diarrheal pathogen affecting humans and a frequent cause of waterborne/foodborne parasitic diseases worldwide. Prevalence of giardiasis is higher in children, living in poor, low hygiene settings in developing countries, and in travelers returning from highly endemic areas. The clinical picture of giardiasis is heterogeneous, with high variability in severity of clinical disease. It can become chronic or be followed by post-infectious sequelae. An alarming increase in cases refractory to the conventional treatment with nitroimidazoles (ie, metronidazole) has been reported in low prevalence settings, such as European Union countries, especially in patients returning from Asia. In view of its relevance, we aim in this review to recapitulate present clinical knowledge about Giardia, with a special focus on the challenge of treatment-refractory giardiasis. We propose a working definition of clinically drug-resistant giardiasis, summarize knowledge regarding resistance mechanisms, and discuss its clinical management according to research-based evidence and medical practice. Advances in development and identification of novel drugs and potential non-pharmacological alternatives are also reviewed with the overall aim to define knowledge gaps and suggest future directions for research.

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Section: Introductionmentioning

confidence: 99%

Treatment-refractory giardiasis: challenges and solutions

Lalle

Hanevik

2018

IDR

108

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“…The MMV Malaria Box molecules ( 4 ) have been extensively studied for their inhibitory potential against asexual and sexual stages of P. falciparum ( 24 ). This valuable antimalarial collection has also been screened against other parasitic species, such as kinetoplastids ( 19 – 21 ), helminths ( 17 ), Babesia ( 67 ), Theileria ( 68 ), Cryptosporidium ( 18 ), Toxoplasma ( 41 ), Giardia ( 69 ), and Entamoeba ( 41 ). These screens primarily focused on determining killing efficacies in whole-organism assays.…”

Section: Discussionmentioning

confidence: 99%

Targeted Phenotypic Screening in Plasmodium falciparum and Toxoplasma gondii Reveals Novel Modes of Action of Medicines for Malaria Venture Malaria Box Molecules

Subramanian

Belekar

Shukla

et al. 2018

mSphere

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The phylum Apicomplexa includes many human and animal pathogens, such as Plasmodium falciparum (human malaria) and Toxoplasma gondii (human and animal toxoplasmosis). Widespread resistance to current antimalarials and the lack of a commercial vaccine necessitate novel pharmacological interventions with distinct modes of action against malaria. For toxoplasmosis, new drugs to effectively eliminate tissue-dwelling latent cysts of the parasite are needed. The Malaria Box antimalarial collection, managed and distributed by the Medicines for Malaria Venture, includes molecules of novel chemical classes with proven antimalarial efficacy. Using targeted phenotypic assays of P. falciparum and T. gondii, we have identified a subset of the Malaria Box molecules as potent inhibitors of plastid segregation and parasite invasion and egress, thereby providing early insights into their probable mode of action. Five molecules that inhibit the egress of both parasites have been identified for further mechanistic studies. Thus, the approach we have used to identify novel molecules with defined modes of action in multiple parasites can expedite the development of pan-active antiparasitic agents.

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“…Comparative analysis showed that the luciferase-based assay described here has a high level of reliability and reproducibility based on the assay of a known standard drug, metronidazole, a previously-known alternative, albendazole, and determination of EC 50 s for selected hits from the Pathogen Box library. This assay overcomes the limitation of drug screening platforms that rely on assessment of parasite numbers without regard to parasite viability [ 27 , 28 ], since only viable parasite cells can produce the ATP required for the D-luciferin reaction.…”

Section: Discussionmentioning

confidence: 99%

“…Semi high-throughput assays using resazurin to measure cell viability [ 26 ] and another based on automated image analysis by cell stained-DAPI signal read-out have also been explored [ 27 ]. Most recently, a digital phase-contrast microscopy morphology-based assay method with enumeration by software was developed, which does not require cell staining [ 28 ]. The morphology-based assay is comparable to the previously reported DAPI stain method, but it relies solely on expensive software to identify and count parasites based on size and morphology [ 27 , 28 ].…”

Section: Introductionmentioning

confidence: 99%

“…Most recently, a digital phase-contrast microscopy morphology-based assay method with enumeration by software was developed, which does not require cell staining [ 28 ]. The morphology-based assay is comparable to the previously reported DAPI stain method, but it relies solely on expensive software to identify and count parasites based on size and morphology [ 27 , 28 ]. Stable expression of Escherichia coli β-glucuronidase A (GusA) as a reporter gene for G .…”

Section: Introductionmentioning

confidence: 99%

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Screening of the Pathogen Box for inhibitors with dual efficacy against Giardia lamblia and Cryptosporidium parvum

et al. 2018

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There is need for a more efficient cell-based assay amenable to high-throughput drug screening against Giardia lamblia. Here, we report the development of a screening method utilizing G. lamblia engineered to express red-shifted firefly luciferase. Parasite growth and replication were quantified using D-luciferin as a substrate in a bioluminescent read-out plateform. This assay was validated for reproducibility and reliability against the Medicines for Malaria Venture (MMV) Pathogen Box compounds. For G. lamblia, forty-three compounds showed ≥ 75% inhibition of parasite growth in the initial screen (16 μM), with fifteen showing ≥ 95% inhibition. The Pathogen Box was also screened against Nanoluciferase expressing (Nluc) C. parvum, yielding 85 compounds with ≥ 75% parasite growth inhibition at 10 μM, with six showing ≥ 95% inhibition. A representative set of seven compounds with activity against both parasites were further analyzed to determine the effective concentration that causes 50% growth inhibition (EC50) and cytotoxicity against mammalian HepG2 cells. Four of the seven compounds were previously known to be effective in treating either Giardia or Cryptosporidium. The remaining three shared no obvious chemical similarity with any previously characterized anti-parasite diarrheal drugs and offer new medicinal chemistry opportunities for therapeutic development. These results suggest that the bioluminescent assays are suitable for large-scale screening of chemical libraries against both C. parvum and G. lamblia.

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A novel in vitro image-based assay identifies new drug leads for giardiasis

Cited by 21 publications

References 51 publications

Treatment-refractory giardiasis: challenges and solutions

Treatment-refractory giardiasis: challenges and solutions

Targeted Phenotypic Screening in Plasmodium falciparum and Toxoplasma gondii Reveals Novel Modes of Action of Medicines for Malaria Venture Malaria Box Molecules

Screening of the Pathogen Box for inhibitors with dual efficacy against Giardia lamblia and Cryptosporidium parvum

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