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Increased Potency and Selectivity for Group III Metabotropic Glutamate Receptor Agonists Binding at Dual sites

Date
2018
Author
Oueslati, Nadia
Cabaye, Alexandre
Tora, Amelie S.
Commare, Bruno
McLean, Heather
Leroux, Frederic R.
Colobert, Francoise
Daniel, Herve
Goupil-Lamy, Anne
Bertrand, Hugues-Olivier
Goudet, Cyril
Pin, Jean-Philippe
Acher, Francine C.
Karaman, Berin
Selvam, Chelliah
Lemasson, Isabelle A.
Brabet, Isabelle
Courtiol, Tiphanie
Cesarini, Sara
McCort-Tranchepain, Isabelle
Rigault, Delphine
Mony, Laetitia
Bessiron, Thomas
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Abstract
A group III metabotropic glutamate (mGlu) receptor agonist (PCEP) was identified by virtual HTS. This orthosteric ligand is composed by an L-AP4-derived fragment that mimics glutamate and a chain that binds into a neighboring pocket, offering possibilities to improve affinity and selectivity. Herein we describe a series of derivatives where the distal chain is replaced by an aromatic or heteroaromatic group. Potent agonists were identified, including some with a mGlu(4) subtype preference, e.g., 17m (LSP1-2111) and 16g (LSP4-2022). Molecular modeling suggests that aromatic functional groups may bind at either one of the two chloride regulatory sites. These agonists may thus be considered as particular bitopic/dualsteric ligands. 17m was shown to reduce GABAergic synaptic transmission at striatopallidal synapses. We now demonstrate its inhibitory effect at glutamatergic parallel fiber-Purkinje cell synapses in the cerebellar cortex. Although these ligands have physicochemical properties that are markedly different from typical CNS drugs, they hold significant therapeutic potential.
URI
http://hdl.handle.net/20.500.12627/93623
https://doi.org/10.1021/acs.jmedchem.7b01438
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Creative Commons Lisansı

İstanbul Üniversitesi Akademik Arşiv Sistemi (ilgili içerikte aksi belirtilmediği sürece) Creative Commons Alıntı-GayriTicari-Türetilemez 4.0 Uluslararası Lisansı ile lisanslanmıştır.

DSpace software copyright © 2002-2016  DuraSpace
Contact Us | Send Feedback
Theme by 
Atmire NV