Si trova su / Altri legami
© Preclinical and clinical development of numerous small molecules is prevented by their poor aqueous solubility, limited absorption, and oral bioavailability. Herein, we disclose a general prodrug approach that converts promising lead compounds into aminoalkoxycarbonyloxymethyl (amino AOCOM) ether–substituted analogues that display significantly improved aqueous solubility and enhanced oral bioavailability, restoring key requirements typical for drug candidate profiles. The prodrug is completely independent of biotransformations and animal–independent because it becomes an active compound via a pH–triggered intramolecular cyclization–elimination reaction. As a proof–of–concept, the utility of this novel amino AOCOM ether prodrug approach was demonstrated on an antimalarial compound series representing a variety of antimalarial 4(1H)–quinolones, which entered and failed preclinical development over the last decade. With the amino AOCOM ether prodrug moiety, the 3–aryl–4(1H)–quinolone preclinical candidate was shown to provide single–dose cures in a rodent malaria model at an oral dose of 3 mg/kg, without the use of an advanced formulation technique.
