Optimization
of Novel α7 Nicotinic Acetylcholine
Receptor Positive Allosteric Modulators and the Discovery of a Preclinical
Development Candidate Molecule (RGH-560)
posted on 2023-11-22, 01:20authored byIstván Ledneczki, Zsolt Némethy, Katalin Dudásné Molnár, Pál Tapolcsányi, Viktor Ilkei, István Vágó, Sándor Kolok, Márta Thán, Judit Laszy, Ottilia Balázs, Balázs Krámos, Áron Szigetvári, Imre Bata, Attila Makó, András Visegrády, László Fodor, Mónika Vastag, György Lévay, Balázs Lendvai, István Greiner, János Éles
During optimization of a previously identified lead compound,
attempts
were made to optimize the reactive indole structural element, the
suboptimal metabolic stability, as well as the low kinetic solubility.
It was concluded that the indole was important for in vitro activity. With the aim of further improvements, more thorough modifications
were also carried out. As a result, a new chemotype (the azetidinespirochromone
family) was identified, which proved to be 1 order of magnitude less
lipophilic retaining the same high level of in vitro potency as the lead series itself, however, with improved metabolic
stability and kinetic solubility. Compound 53 showed
the most balanced physicochemical and pharmacological profile with
significant in vivo efficacy in the scopolamine-induced
amnesia test. Based on these promising results, cognitive enhancement
through the positive modulation of α7 nAChRs appears to be a
viable approach. Compound 53 was selected to be a preclinical
development candidate (as RGH-560).