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Characterization of conantokin Rl‐A: molecular phylogeny as structure/function study
Authors:Konkallu H. Gowd  Maren Watkins  Vernon D. Twede  Grzegorz W. Bulaj  Baldomero M. Olivera
Affiliation:1. Department of Biology, University of Utah, Salt Lake City, Utah 84112, USA;2. Department of Medicinal Chemistry, University of Utah, Salt Lake City, Utah 84112, USA
Abstract:A multidisciplinary strategy for discovery of new Conus venom peptides combines molecular genetics and phylogenetics with peptide chemistry and neuropharmacology. Here we describe application of this approach to the conantokin family of conopeptides targeting NMDA receptors. A new conantokin from Conus rolani, ConRl‐A, was identified using molecular phylogeny and subsequently synthesized and functionally characterized. ConRl‐A is a 24‐residue peptide containing three γ‐carboxyglutamic acid residues with a number of unique sequence features compared to conantokins previously characterized. The HPLC elution of ConRl‐A suggested that this peptide exists as two distinct, slowly exchanging conformers. ConRl‐A is predominantly helical (estimated helicity of 50%), both in the presence and absence of Ca++. The order of potency for blocking the four NMDA receptor subtypes by ConRl‐A was NR2B > NR2D > NR2A > NR2C. This peptide has a greater discrimination between NR2B and NR2C than any other ligand reported so far. In summary, ConRl‐A is a new member of the conantokin family that expands our understanding of structure/function of this group of peptidic ligands targeted to NMDA receptors. Thus, incorporating phylogeny in the discovery of novel ligands for the given family of ion channels or receptors is an efficient means of exploring the megadiverse group of peptides from the genus Conus. Copyright © 2010 European Peptide Society and John Wiley & Sons, Ltd.
Keywords:conantokin  molecular phylogeny  conformational interconversion  helical peptide  electrophysiology
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