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Publication : Age-related decline of the acute local inflammation response: a mitigating role for the adenosine A<sub>2A</sub> receptor.

First Author  Laflamme C Year  2017
Journal  Aging (Albany NY) Volume  9
Issue  10 Pages  2083-2097
PubMed ID  29064819 Mgi Jnum  J:274143
Mgi Id  MGI:6296679 Doi  10.18632/aging.101303
Citation  Laflamme C, et al. (2017) Age-related decline of the acute local inflammation response: a mitigating role for the adenosine A2A receptor. Aging (Albany NY) 9(10):2083-2097
abstractText  Aging is accompanied by an increase in markers of innate immunity. How aging affects neutrophil functions remains of debate.The adenosine A2A receptor (A2AR), essential to the resolution of inflammation, modulates neutrophil functions. We sought to determine whether or not A2AR protects against the effects of aging. We monitored neutrophil influx, viability, and activation as well as cytokine accumulation in wild-type (WT) and A2AR-knockout mice (KO) at three different ages.Several readouts decreased with aging: neutrophil counts in dorsal air pouches (by up to 55%), neutrophil viability (by up to 56%), elastase and total protein in exudates (by up to 80%), and local levels of cytokines (by up to 90%). Each of these parameters was significantly more affected in A2AR-KO mice. CXCL1-3 levels were largely unaffected. The effects of aging were not observed systemically. Preventing neutrophil influx into the air pouch caused a comparable cytokine pattern in young WT mice. Gene expression (mRNA) in leukocytes was affected, with CXCL1 and CCL4 increasing and with TNF and IL-1alpha decreasing.ConclusionAging has deleterious effects on the acute inflammatory response and neutrophil-related activities, and defective migration appears as an important factor. A functional A2AR signaling pathway delays some of these.
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