Exposure of resting endothelial cells to TNF-α or LPS leads to increased expression of the P2Y6 purinergic receptor. Simultaneous or subsequent injury to the endothelium promotes the release of UTP/UDP the endogenous ligands of the P2Y6 receptor. These 2 events serve to up-regulate NF-KB signaling leading to increased IL-8 and VCAM-1 expression to collectively enhance tissue inflammation. This model was derived from experiments by Riegel and colleagues1 demonstrating that genetic removal or pharmacologic inhibition of P2Y6 lead to attenuation of these pathways.

Exposure of resting endothelial cells to TNF-α or LPS leads to increased expression of the P2Y6 purinergic receptor. Simultaneous or subsequent injury to the endothelium promotes the release of UTP/UDP the endogenous ligands of the P2Y6 receptor. These 2 events serve to up-regulate NF-KB signaling leading to increased IL-8 and VCAM-1 expression to collectively enhance tissue inflammation. This model was derived from experiments by Riegel and colleagues demonstrating that genetic removal or pharmacologic inhibition of P2Y6 lead to attenuation of these pathways.

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