| Literature DB >> 32534072 |
Rosanna Matucci1, Cristina Bellucci2, Maria Vittoria Martino2, Marta Nesi3, Dina Manetti2, Jessica Welzel4, Ulrike Bartz5, Janine Holze4, Christian Tränkle4, Klaus Mohr4, Angelica Mazzolari6, Giulio Vistoli6, Silvia Dei2, Elisabetta Teodori2, Maria Novella Romanelli2.
Abstract
Although agonists and antagonists of muscarinic receptors have been known for long time, there is renewed interest in compounds (such as allosteric or bitopic ligands, or biased agonists) able to differently and selectively modulate these receptors. As a continuation of our previous research, we designed a new series of dimers of the well-known cholinergic agonist carbachol. The new compounds were tested on the five cloned human muscarinic receptors (hM1-5) expressed in CHO cells by means of equilibrium binding experiments, showing a dependence of the binding affinity on the length and position of the linker connecting the two monomers. Kinetic binding studies revealed that some of the tested compounds were able to slow the rate of NMS dissociation, suggesting allosteric behavior, also supported by docking simulations. Assessment of ERK1/2 phosphorylation on hM1, hM2 and hM3 activation showed that the new compounds are endowed with muscarinic antagonist properties. At hM2 receptors, some compounds were able to stimulate GTPγS binding but not cAMP accumulation, suggesting a biased behavior. Classification, Molecular and cellular pharmacology.Entities:
Keywords: Acethylcholine chloride; Allosteric modulation; Atropine sulphate; Carbachol chloride; Carbachol dimers; Gallamine triethiodide; Hexamethonium chloride; McN-A-343 chloride; Muscarinic acetylcholine receptor (mAChR); PubChem CID: 5831; PubChem CID: 5926; PubChem CID: 6060; PubChem CID: 6172; PubChem CID: 64663; PubChem CID: 93550
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Year: 2020 PMID: 32534072 DOI: 10.1016/j.ejphar.2020.173183
Source DB: PubMed Journal: Eur J Pharmacol ISSN: 0014-2999 Impact factor: 4.432