Design of Novel Series of Antimalarial PMX Inhibitors with Increased Half-Life via Molecular Property Optimization.

Authors :: Sakata K
Lowe MA
Xuan M
Bruffaerts J
Stasi LP
Lallemand B
Cardenas A
Taylor RD
Vidler LR
King L
Valentin JP
Laleu B
de Haro T
Source :: ACS medicinal chemistry letters [ACS Med Chem Lett] 2023 Oct 20; Vol. 14 (11), pp. 1582-1588. Date of Electronic Publication: 2023 Oct 20 (Print Publication: 2023).
Publication Year :: 2023
Abstract: Plasmepsin X (PMX) has been identified as a multistage antimalarial target. PMX is a malarial aspartyl protease essential for merozoite egress from infected red blood cells and invasion of the host erythrocytes. Previously, we reported the identification of PMX inhibitors by structure-based optimization of a cyclic guanidine core. Preclinical assessment of UCB7362 , which displayed both in vitro and in vivo antimalarial activity, revealed a suboptimal dose paradigm (once daily dosing of 50 mg for 7 days for treatment of uncomplicated malaria) relative to current standard of care (three-dose regime). We report here the efforts toward extending the half-life ( t <subscript>1/2</subscript> ) by reducing metabolic clearance and increasing volume of distribution ( V ss). Our efforts culminated in the identification of a biaryl series, with an expected longer t <subscript>1/2</subscript> in human than UCB7362 while maintaining a similar in vitro off-target hit rate.<br />Competing Interests: The authors declare no competing financial interest.<br /> (© 2023 American Chemical Society.)

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