A Ligand-Mimetic Model for Constitutive Activation of the Melanocortin-1 Receptor | Zendy

Dongsi Lu | Zendy; Dag Inge Våge | Zendy; Roger D. Cone | Zendy

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A Ligand-Mimetic Model for Constitutive Activation of the Melanocortin-1 Receptor

Author(s) -

Dongsi Lu,

Dag Inge Våge,

Roger D. Cone

Publication year - 1998

Publication title -

molecular endocrinology

Language(s) - English

Resource type - Journals

eISSN - 1944-9917

pISSN - 0888-8809

DOI - 10.1210/mend.12.4.0091

Subject(s) - biology , receptor , transmembrane domain , transmembrane protein , melanocortin , microbiology and biotechnology , agonist , ligand (biochemistry) , 5 ht5a receptor , g protein coupled receptor , enzyme linked receptor , biophysics , biochemistry

Dark coat color in the mouse and fox results from constitutively activated melanocortin-1 receptors. Receptor mutations in the mouse (E92K, L98P), cow (L99P), fox (C125R), and sheep (D119N) cluster near the membrane/extracellular junctions of the second and third transmembrane domains, an acidic domain that is the likely site of electrostatic interaction with an arginine residue in the ligand, alpha-MSH. For transmembrane residues E92, D119, and C125, conversion to a basic residue is required for constitutive activation. Unlike constitutively activating mutations in many G protein-coupled receptors that increase agonist efficacy and affinity, these MC1-R mutations have the opposite effect. Therefore, these mutations do not activate the receptor by directly disrupting intramolecular constraints on formation of the active high-affinity state, R*, but do so indirectly by mimicking ligand binding.

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