1. Academic Validation
  2. Cutting edge: identification of a novel chemokine receptor that binds dendritic cell- and T cell-active chemokines including ELC, SLC, and TECK

Cutting edge: identification of a novel chemokine receptor that binds dendritic cell- and T cell-active chemokines including ELC, SLC, and TECK

  • J Immunol. 2000 Mar 15;164(6):2851-6. doi: 10.4049/jimmunol.164.6.2851.
J Gosling 1 D J Dairaghi Y Wang M Hanley D Talbot Z Miao T J Schall
Affiliations

Affiliation

  • 1 Divisions of Discovery Biology and Molecular Pharmacology, ChemoCentryx, San Carlos, CA 94070, USA.
Abstract

Searching for new receptors of dendritic cell- and T cell-active chemokines, we used a combination of techniques to interrogate orphan chemokine receptors. We report here on human CCX CKR, previously represented only by noncontiguous expressed sequence tags homologous to bovine PPR1, a putative gustatory receptor. We employed a two-tiered process of ligand assignment, where immobilized chemokines constructed on stalks (stalkokines) were used as bait for adhesion of cells expressing CCX CKR. These cells adhered to stalkokines representing ELC, a chemokine previously thought to bind only CCR7. Adhesion was abolished in the presence of soluble ELC, SLC (CCR7 ligands), and TECK (a CCR9 ligand). Complete ligand profiles were further determined by radiolabeled ligand binding and competition with >80 chemokines. ELC, SLC, and TECK comprised high affinity ligands (IC50 <15 nM); lower affinity ligands include BLC and vMIP-II (IC50 <150 nM). With its high affinity for CC Chemokines and homology to CC receptors, we provisionally designate this new receptor CCR10.

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