High Affinity Fluorescent Probe for Proteinase-Activated Receptor 2 (PAR2)

Overview

Journal ACS Med Chem Lett

Publisher American Chemical Society

Specialty Chemistry

Date 2019 Jul 18

PMID 31312406

Citations 1

Authors

Jordan C LeSarge

Pierre Thibeault

Mark Milne

Rithwik Ramachandran

Leonard G Luyt

Affiliations

Soon will be listed here.

Abstract

PAR2 is a proteolytically activated G protein-coupled receptor (GPCR) that is implicated in various cancers and inflammatory diseases. Ligands with low nanomolar affinity for PAR2 have been developed, but there is a paucity of research on the development of PAR2-targeting imaging probes. Here, we report the development of seven novel PAR2-targeting compounds. Four of these compounds are highly potent and selective PAR2-targeting peptides (EC = 10 to 23 nM) that have a primary amine handle available for facile conjugation to various imaging components. We describe a peptide of the sequence Isox-Cha-Chg-ARK(Sulfo-Cy5)-NH as the most potent and highest affinity PAR2-selective fluorescent probe reported to date (EC = 16 nM, = 38 nM). This compound has a greater than 10-fold increase in potency and binding affinity for PAR2 compared to the leading previously reported probe and is conjugated to a red-shifted fluorophore, enabling and studies.

Citing Articles

Role of the Helix-8 and C-Terminal Tail in Regulating Proteinase Activated Receptor 2 Signaling.

Thibeault P, Ramachandran R ACS Pharmacol Transl Sci. 2020; 3(5):868-882.

PMID: 33073187 PMC: 7551709. DOI: 10.1021/acsptsci.0c00039.

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