Figure 5.
Figure 5. Proposed model of leukocyte-endothelial cross-talk at sites of inflammation. In areas of ongoing inflammation, diminished oxygen supply coordinates the induction of CD39 and CD73. At such sites, activated PMNs provide a readily available extracellular source of ATP, which through 2 enzymatic steps is metabolized to adenosine. Adenosine generated in this fashion is available for activation of PMN adenosine receptors, particularly the AdoRA2A and AdoRA2B, leading to decreased in PMN adhesion and transmigration. As such, this form of leukocyte-endothelial cell cross-talk may provide an innate mechanism to dampen ongoing inflammatory responses.

Proposed model of leukocyte-endothelial cross-talk at sites of inflammation. In areas of ongoing inflammation, diminished oxygen supply coordinates the induction of CD39 and CD73. At such sites, activated PMNs provide a readily available extracellular source of ATP, which through 2 enzymatic steps is metabolized to adenosine. Adenosine generated in this fashion is available for activation of PMN adenosine receptors, particularly the AdoRA2A and AdoRA2B, leading to decreased in PMN adhesion and transmigration. As such, this form of leukocyte-endothelial cell cross-talk may provide an innate mechanism to dampen ongoing inflammatory responses.

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