- Présentation
- Équipes de Recherche
- Biogéochimie moléculaire
- [BCB] Biométaux et Chimie Biologique
- [CLIC] Coordination, Ligands, Interactions et Catalyse
- [CBMB] Chimie et Biochimie de Molécules Bioactives
- [LCQ] Chimie quantique
- [LECPCS] Electrochimie et Chimie Physique du Corps Solide
- [COSyS] Catalyse Organométallique, Synthèse organique et Santé
- [SOPhy] Synthèse Organique & Phytochimie
- [LSAMM] Synthèse des Assemblages Moléculaires Multifonctionnels
- [LCSOM] Chimie et Systémique Organo-Métalliques
- [CBAT] Chimie Biologique et Applications Thérapeutiques
- [ECMC] Confinement Moléculaire et Catalyse
- [POMAM] Propriétés Optiques et Magnétiques des Architectures Moléculaires
- Biophysique des membranes et RMN
- [IFM] Laboratoire d’Ingénierie des Fonctions Moléculaires
- [SRCO] Synthèse, Réactivité et Catalyse Organométalliques
- [OMECA] Objets, MEtaux et CAtalyse
- [SOCAT] Synthèse Organométallique et CATalyse
- Services scientifiques
- Actualités de l'institut
- Agenda - Conférences
- Annuaires CNRS et Université
Résumé: Une description en principe exacte des excitations électroniques...
Abstract: CPPs, or Cell-Penetrating Peptides, offer invaluable utility in...
Cell [IFM]
- Catégorie(s) : Publications récentes
Tweet:
The IFM team provides the first structural interpretation of the allosteric modulation at the α7 nicotinic acetylcholine receptor in collaboration with world-renowned structural biologists and electro physiologists from the University of California San Diego (USA) and the Mayo Clinic College of Medicine and Science in Rochester (USA). These results appeared in Cell (IF 66,85) have important implications for the development of new drug therapies for brain disorders.
Graphical Abstract:
The α7 nicotinic acetylcholine receptor is a pentameric ligand-gated ion channel that plays an important role in cholinergic signaling throughout the nervous system. Its unique physiological characteristics and implications in neurological disorders and inflammation make it a promising but challenging therapeutic target. Positive allosteric modulators overcome limitations of traditional α7 agonists, but their potentiation mechanisms remain unclear. Here, we present high-resolution structures of α7-modulator complexes, revealing partially overlapping binding sites but varying conformational states. Structure-guided functional and computational tests suggest that differences in modulator activity arise from the stable rotation of a channel gating residue out of the pore. We extend the study using a time-resolved cryoelectron microscopy (cryo-EM) approach to reveal asymmetric state transitions for this homomeric channel and find that a modulator with allosteric agonist activity exploits a distinct channel-gating mechanism. These results define mechanisms of α7 allosteric modulation and activation with implications across the pentameric receptor superfamily.
Reference:
Sean Burke, Mariia Avstrikova, Coleen Noviello, Nuriya Mukhtasimova, Jean-Pierre Changeux, Ganesh Thakur, Steven Sine, Marco Cecchini and Ryan Hibbs
Structural mechanisms of α7 nicotinic receptor allosteric modulation and activation
Cell 2024, DOI: https://doi.org/10.1016/j.cell.2024.01.032
Contact:
Marco Cecchini, équipe IFM, Institut de Chimie (UMR 7177).