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Potent and Selective Oxidatively Labile Ether‐Based Prodrugs through Late‐Stage Boronate Incorporation

Paul Geaneotes, Chasity P. Janosko, Cephas Afeke, Alexander Deiters, Paul E. Floreancig

2024Angewandte Chemie International Edition12 citationsDOIOpen Access PDF

Abstract

This manuscript describes a new strategy for prodrug synthesis in which a relatively inert ether group is introduced at an early stage in a synthetic sequence and functionalized in the final step to introduce a prodrug-activating group through a chemoselective process. Boryl allyloxy (BAO) ether groups are synthesized through several metal-mediated processes to form entities that are readily cleaved under oxidative conditions commonly found in cancer cells. The high cleavage propensity of the BAO group allows for ether cleavage, making these compounds substantially more hydrolytically stable in comparison to acyl-linked prodrugs while retaining the ability to release alcohols. We report the preparation of prodrug analogues of the natural products camptothecin and pederin from acetal precursors that serve as protecting groups in their synthetic sequences. The BAO acetal groups cleave in the presence of hydrogen peroxide to release the cytotoxic agents. The pederin-based prodrug shows dramatically greater cytotoxicity than negative controls and outstanding selectivity and potency toward cancer cell lines in comparison to non-cancerous cell lines. This late-stage functionalization approach to prodrug synthesis should be applicable to numerous systems that can be accessed through chemoselective processes.

Topics & Concepts

ProdrugChemistryEtherAcetalCombinatorial chemistryWilliamson ether synthesisCytotoxicityCleavage (geology)Ether cleavageCleaveStereochemistryOrganic chemistryBiochemistryIn vitroEnzymeBiologyPaleontologyFracture (geology)Cancer therapeutics and mechanismsSynthetic Organic Chemistry MethodsPeptidase Inhibition and Analysis
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