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Publication : Increased inflammation in mice deficient for the chemokine decoy receptor D6.

First Author  Martinez de la Torre Y Year  2005
Journal  Eur J Immunol Volume  35
Issue  5 Pages  1342-6
PubMed ID  15789340 Mgi Jnum  J:97806
Mgi Id  MGI:3576431 Doi  10.1002/eji.200526114
Citation  de la Torre YM, et al. (2005) Increased inflammation in mice deficient for the chemokine decoy receptor D6. Eur J Immunol 35(5):1342-6
abstractText  Chemokines are chemotactic cytokines with a key role in the control of cell trafficking and positioning under homeostatic and inflammatory conditions. D6 is a promiscuous 7-transmembrane-domain receptor expressed on lymphatic vessels which recognizes most inflammatory, but not homeostatic, CC chemokines. In vitro experiments demonstrated that D6 is unable to signal after ligand engagement, and it is structurally adapted to sustain rapid and efficient ligand internalization and degradation. These unique functional properties lead to the hypothesis that D6 may be involved in the control of inflammation by acting as a decoy and scavenger receptor for inflammatory chemokines. Consistent with this hypothesis, here we report that D6(-/-) mice showed an anticipated and exacerbated inflammatory response in a model of skin inflammation. Moreover, the absence of D6 resulted in increase cellularity and inflammatory-chemokine levels in draining lymph nodes. Thus, D6 is a decoy receptor structurally adapted and strategically located to tune tissue inflammation and control transfer of inflammatory chemokines to draining lymph nodes.
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