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Receptor Activity-modifying Proteins 2 and 3 Generate Adrenomedullin Receptor Subtypes with Distinct Molecular Properties
Authors:Harriet A. Watkins  Madhuri Chakravarthy  Rekhati S. Abhayawardana  Joseph J. Gingell  Michael Garelja  Meenakshi Pardamwar  James M. W. R. McElhinney  Alex Lathbridge  Arran Constantine  Paul W. R. Harris  Tsz-Ying Yuen  Margaret A. Brimble  James Barwell  David R. Poyner  Michael J. Woolley  Alex C. Conner  Augen A. Pioszak  Christopher A. Reynolds  Debbie L. Hay
Abstract:Adrenomedullin (AM) is a peptide hormone with numerous effects in the vascular systems. AM signals through the AM1 and AM2 receptors formed by the obligate heterodimerization of a G protein-coupled receptor, the calcitonin receptor-like receptor (CLR), and receptor activity-modifying proteins 2 and 3 (RAMP2 and RAMP3), respectively. These different CLR-RAMP interactions yield discrete receptor pharmacology and physiological effects. The effective design of therapeutics that target the individual AM receptors is dependent on understanding the molecular details of the effects of RAMPs on CLR. To understand the role of RAMP2 and -3 on the activation and conformation of the CLR subunit of AM receptors, we mutated 68 individual amino acids in the juxtamembrane region of CLR, a key region for activation of AM receptors, and determined the effects on cAMP signaling. Sixteen CLR mutations had differential effects between the AM1 and AM2 receptors. Accompanying this, independent molecular modeling of the full-length AM-bound AM1 and AM2 receptors predicted differences in the binding pocket and differences in the electrostatic potential of the two AM receptors. Druggability analysis indicated unique features that could be used to develop selective small molecule ligands for each receptor. The interaction of RAMP2 or RAMP3 with CLR induces conformational variation in the juxtamembrane region, yielding distinct binding pockets, probably via an allosteric mechanism. These subtype-specific differences have implications for the design of therapeutics aimed at specific AM receptors and for understanding the mechanisms by which accessory proteins affect G protein-coupled receptor function.
Keywords:allosteric regulation   cardiovascular disease   conformational change   G protein-coupled receptor (GPCR)   molecular modeling   GPCR   RAMP   adrenomedullin   extracellular loops   receptor activity-modifying protein
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