Abstract
Chemokine receptors guide cell migration by responding to local chemokine gradients during immune surveillance and inflammation. Similar to other G protein-coupled receptors, chemokine receptors can form oligomeric complexes that might have distinct pharmacological and biochemical properties as compared to their individual constituents. The majority of evidence for chemokine receptor oligomers came from transfected cells using tagged receptors to monitor their close proximity or physical association. However, translation of these observations to (patho)-physiological consequences is puzzling for the majority of chemokine receptor oligomers due to experimental limitations and challenges to distinguish oligomer- from downstream signaling-mediated crosstalk. Recent methodological advances allow in situ validation of chemokine receptor oligomers in native cells, disruption of oligomers, and detection of oligomer-mediated signaling. Chemokine receptor oligomerization modulates cell migration in (patho)-physiology and consequently offers novel therapeutic targets.
| Original language | English |
|---|---|
| Title of host publication | G-Protein-Coupled Receptor Dimers |
| Editors | Katherine Herrick-Davis, Graeme Milligan, Giuseppe Di Giovanni |
| Publisher | Humana Press |
| Chapter | 9 |
| Pages | 233-272 |
| Number of pages | 40 |
| ISBN (Electronic) | 9783319601748 |
| ISBN (Print) | 9783319601724, 9783319867953 |
| DOIs | |
| Publication status | Published - 2017 |
Publication series
| Name | The Receptors |
|---|---|
| Publisher | Humana Press |
| Volume | 33 |
UN SDGs
This output contributes to the following UN Sustainable Development Goals (SDGs)
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SDG 3 Good Health and Well-being
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