Development of a Potent and Selective G2A (GPR132) Agonist
journal contribution
posted on 2024-06-25, 17:09 authored by Victor Hernandez-Olmos, Jan Heering, Beatrice Marinescu, Tina Schermeng, Vladimir V. Ivanov, Yurii S. Moroz, Sheila Nevermann, Marius Mathes, Johanna H. M. Ehrler, Mohamad Wessam Alnouri, Markus Wolf, Alicia S. Haydo, Tessa Schmachtel, Andrea Zaliani, Georg Höfner, Astrid Kaiser, Manfred Schubert-Zsilavecz, Annette G. Beck-Sickinger, Stefan Offermanns, Philipp Gribbon, Michael A. Rieger, Daniel Merk, Marco Sisignano, Dieter Steinhilber, Ewgenij ProschakG protein-coupled
receptor G2A was postulated to be a promising
target for the development of new therapeutics in neuropathic pain,
acute myeloid leukemia, and inflammation. However, there is still
a lack of potent, selective, and drug-like G2A agonists to be used
as a chemical tool or as the starting matter for the development of
drugs. In this work, we present the discovery and structure–activity
relationship elucidation of a new potent and selective G2A agonist
scaffold. Systematic optimization resulted in (3-(pyridin-3-ylmethoxy)benzoyl)-d-phenylalanine (T-10418) exhibiting higher
potency than the reference and natural ligand 9-HODE and high selectivity
among G protein-coupled receptors. With its favorable activity, a
clean selectivity profile, excellent solubility, and high metabolic
stability, T-10418 qualifies as a pharmacological tool to investigate
the effects of G2A activation.
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systematic optimization resultednatural ligand 9high metabolic stabilityexhibiting higher potencyclean selectivity profileagonist g proteinacute myeloid leukemialike g2a agonistscoupled receptor g2a3 -( pyriding2a activationcoupled receptorsstarting matterselective g2apromising targetpharmacological toolnew therapeuticsneuropathic painfavorable activityexcellent solubilitychemical tool>- phenylalanine
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