A previous phenotypic screening campaign led to the identification of a quinazoline derivative with promising activity against . Follow-up studies of the antischistosomal potential of this candidate are presented here. The studies in a mouse model show a significant reduction of total worms and a complete disappearance of immature eggs when administered concomitantly with praziquantel in comparison with the administration of praziquantel alone. This fact is of utmost importance because eggs are responsible for the pathology and transmission of the disease. Subsequently, the chemical optimisation of the structure in order to improve the metabolic stability of the parent compound was carried out leading to derivatives with improved drug-like properties. Additionally, the putative target of this new class of antischistosomal compounds was envisaged by using computational tools and the binding mode to the target enzyme, aldose reductase, was proposed.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7717570PMC
http://dx.doi.org/10.1080/14756366.2020.1712595DOI Listing

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