Chemokine receptors (version 2020.5) in the IUPHAR/BPS Guide to Pharmacology Database

Francoise Bachelerie; Adit Ben-Baruch; Amanda M. Burkhardt; Israel F. Charo; Christophe Combadiere; Reinhold Förster; Joshua M. Farber; Gerard J. Graham; Rebecca Hills; Richard Horuk; Massimo Locati; Andrew D. Luster; Alberto Mantovani; Kouji Matsushima; Amy E. Monaghan; Georgios L. Moschovakis; Philip M. Murphy; Robert J. B. Nibbs; Hisayuki Nomiyama; Joost J. Oppenheim; Christine A. Power; Amanda E. I. Proudfoot; Mette M. Rosenkilde; Antal Rot; Silvano Sozzani; Alexander H. Sparre-Ulrich; Marcus Thelen; Mohib Uddin; Osamu Yoshie; Albert Zlotnik

doi:10.2218/gtopdb/F14/2020.5

Francoise Bachelerie Institut Pasteur
Adit Ben-Baruch Tel Aviv University
Amanda M. Burkhardt University of California, Irvine
Israel F. Charo Gladstone Institutes
Christophe Combadiere INSERM
Reinhold Förster Hannover Medical School
Joshua M. Farber National Institute of Allergy and Infectious Diseases
Gerard J. Graham University of Glasgow
Rebecca Hills University of Edinburgh
Richard Horuk Berlex Laboratories
Massimo Locati University of Milan https://orcid.org/0000-0003-3077-590X
Andrew D. Luster Massachusetts General Hospital
Alberto Mantovani University of Milan
Kouji Matsushima University of Tokyo
Amy E. Monaghan University of Edinburgh
Georgios L. Moschovakis Hannover Medical School
Philip M. Murphy National Institutes of Health
Robert J. B. Nibbs University of Glasgow
Hisayuki Nomiyama Kumamoto University Graduate School of Medical Sciences
Joost J. Oppenheim Frederick National Laboratory for Cancer Research
Christine A. Power Merck Serono Geneva Research Center
Amanda E. I. Proudfoot Merck Serono Geneva Research Center
Mette M. Rosenkilde Panum Instituttet
Antal Rot University of Birmingham
Silvano Sozzani University of Brescia
Alexander H. Sparre-Ulrich University of Copenhagen
Marcus Thelen Institute for Research in Biomedicine
Mohib Uddin AstraZeneca https://orcid.org/0000-0002-2412-2657
Osamu Yoshie Kinki University
Albert Zlotnik University of California Irvine

Abstract

Chemokine receptors (nomenclature as agreed by the NC-IUPHAR Subcommittee on Chemokine Receptors [431, 430, 32]) comprise a large subfamily of 7TM proteins that bind one or more chemokines, a large family of small cytokines typically possessing chemotactic activity for leukocytes. Additional hematopoietic and non-hematopoietic roles have been identified for many chemokines in the areas of embryonic development, immune cell proliferation, activation and death, viral infection, and as antibiotics, among others. Chemokine receptors can be divided by function into two main groups: G protein-coupled chemokine receptors, which mediate leukocyte trafficking, and "Atypical chemokine receptors", which may signal through non-G protein-coupled mechanisms and act as chemokine scavengers to downregulate inflammation or shape chemokine gradients [32].

Chemokines in turn can be divided by structure into four subclasses by the number and arrangement of conserved cysteines. CC (also known as β-chemokines; n= 28), CXC (also known as α-chemokines; n= 17) and CX3C (n= 1) chemokines all have four conserved cysteines, with zero, one and three amino acids separating the first two cysteines respectively. C chemokines (n= 2) have only the second and fourth cysteines found in other chemokines. Chemokines can also be classified by function into homeostatic and inflammatory subgroups. Most chemokine receptors are able to bind multiple high-affinity chemokine ligands, but the ligands for a given receptor are almost always restricted to the same structural subclass. Most chemokines bind to more than one receptor subtype. Receptors for inflammatory chemokines are typically highly promiscuous with regard to ligand specificity, and may lack a selective endogenous ligand. G protein-coupled chemokine receptors are named acccording to the class of chemokines bound, whereas ACKR is the root acronym for atypical chemokine receptors [33]. There can be substantial cross-species differences in the sequences of both chemokines and chemokine receptors, and in the pharmacology and biology of chemokine receptors. Endogenous and microbial non-chemokine ligands have also been identified for chemokine receptors. Many chemokine receptors function as HIV co-receptors, but CCR5 is the only one demonstrated to play an essential role in HIV/AIDS pathogenesis. The tables include both standard chemokine receptor names [684] and aliases.

DOI: https://doi.org/10.2218/gtopdb/F14/2020.5