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  4. Translation of liver stage activity of M5717, a; Plasmodium; elongation factor 2 inhibitor: from bench to bedside
 
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Translation of liver stage activity of M5717, a; Plasmodium; elongation factor 2 inhibitor: from bench to bedside

Date Issued
2022-01-01
Author(s)
Khandelwal, A.
Arez, F.
Alves, P. M.
Badolo, L.
Brito, C.
Fischli, C.  
Fontinha, D.
Oeuvray, C.
Prudêncio, M.
Rottmann, M.  
Wilkins, J.
Yalkinoglu, Ö.
Bagchus, W. M.
Spangenberg, T.
DOI
10.1186/s12936-022-04171-0
Abstract
BACKGROUND: Targeting the asymptomatic liver stage of Plasmodium infection through chemoprevention could become a key intervention to reduce malaria-associated incidence and mortality. METHODS: M5717, a Plasmodium elongation factor 2 inhibitor, was assessed in vitro and in vivo with readily accessible Plasmodium berghei parasites. In an animal refinement, reduction, replacement approach, the in vitro IC99 value was used to feed a Population Pharmacokinetics modelling and simulation approach to determine meaningful effective doses for a subsequent Plasmodium sporozoite-induced volunteer infection study. RESULTS: Doses of 100 and 200 mg would provide exposures exceeding IC99 in 96 and 100% of the simulated population, respectively. CONCLUSIONS: This approach has the potential to accelerate the search for new anti-malarials, to reduce the number of healthy volunteers needed in a clinical study and decrease and refine the animal use in the preclinical phase.
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s12936-022-04171-0

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