Litcius/Paper detail

Identification and Optimization of EphA2-Selective Bicycles for the Delivery of Cytotoxic Payloads

Gemma Mudd, Amy Brown, Liuhong Chen, Katerine Van Rietschoten, Sophie Watcham, Daniel P. Teufel, Silvia Pavan, Rachid Lani, Philip Huxley, Gavin Bennett

2020Journal of Medicinal Chemistry79 citationsDOIOpen Access PDF

Abstract

Bicycles are constrained bicyclic peptides that represent a promising binding modality for use in targeted drug conjugates. A phage display screen against EphA2, a receptor tyrosine kinase highly expressed in a number of solid tumors, identified a number of Bicycle families with low nanomolar affinity. A Bicycle toxin conjugate (BTC) was generated by derivatization of one of these Bicycles with the potent cytotoxin DM1 via a cleavable linker. This BTC demonstrated potent antitumor activity in vivo but was poorly tolerated, which was hypothesized to be the result of undesired liver uptake caused by poor physicochemical properties. Chemical optimization of a second Bicycle, guided by structural biology, provided a high affinity, metabolically stable Bicycle with improved physicochemical properties. A BTC incorporating this Bicycle also demonstrated potent antitumor activity and was very well tolerated when compared to the initial BTC. Phage display selection followed by chemical optimization of Bicycles can deliver potent drug conjugates with favorable pharmaceutical properties.

Topics & Concepts

LinkerChemistryIn vivoConjugatePhage displayPharmacologyLead compoundChemical synthesisDrugStructure–activity relationshipCombinatorial chemistryBiochemistryIn vitroBiologyPeptideComputer scienceMathematicsMathematical analysisOperating systemBiotechnologyAxon Guidance and Neuronal SignalingBiochemical and Structural CharacterizationMonoclonal and Polyclonal Antibodies Research