Discovery of an In Vitro and In Vivo Potent Nicotinic α7 Positive Allosteric Modulator Clinical Candidate Molecule (RGH-857)

  • J Med Chem. 2026 Jan 8;69(1):305-329. doi: 10.1021/acs.jmedchem.5c02408.
István Ledneczki  1 Pál Tapolcsányi  1 Eszter Gábor  1 István Vágó  1 Áron Szigetvári  1 Balázs Krámos  1 Réka Mohácsi  1 Sándor Kolok  1 Márta Thán  1 György Lévay  1 Balázs Lendvai  1 István Greiner  1 Zsolt Némethy  1 János Éles  1
Affiliations
  • 1. Gedeon Richter Plc., 19-21 Gyömrői út, Budapest H-1103, Hungary.
Abstract

While identifying α7 nACh receptor positive allosteric modulators, a novel scaffold (1,1-dioxo-thiadiazine core) emerged from our HTS campaign, exhibiting unusually low lipophilicity compared to Other screening hits. During the hit-to-lead optimization, the importance of different structural elements was evaluated. Upon combination of the best building blocks, first a lead molecule (25), then after a subsequent lead optimization, a clinical candidate compound (51, RGH-857) was identified. Having the most balanced physicochemical and in vitro pharmacological profile combined with significant in vivo efficacy in models of scopolamine-induced amnesia and natural forgetting, our results suggest that cognitive enhancement through the positive modulation of α7 nAChRs can be a viable approach to targeting cognitive decline.

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