UDP-glucose promotes neutrophil recruitment in the lung

JULIANA SESMA; CLARISSA D. WEITZER; ALESSANDRA LIVRAGHI-BUTRICO; HONG DANG; SCOTT DONALDSON; NEIL E. ALEXIS; KENNETH A. JACOBSON; T. KENDALL HARDEN; EDUARDO R. LAZAROWSKI

PURINERGIC SIGNALLING

SPRINGER

Lugar: Berlin; Año: 2016

1573-9538

In addition to their role in glycosylation reactions, UDP-sugars are released from cells and activate widely distributed cell surface P2Y14 receptors (P2Y14R). However, the physiological/pathophysiological consequences of UDP-sugar release are incompletely defined. Here, we report that UDP-glucose levels are abnormally elevated in lung secretions from patients with cystic fibrosis (CF) as well as in a mouse model of CF-like disease, the βENaC transgenic (Tg) mouse. Instillation of UDP-glucose into wild-type mouse tracheas resulted in enhanced neutrophil lung recruitment, and this effect was nearly abolished when UDP-glucose was co-instilled with the P2Y14R antagonist PPTN [4-(piperidin-4-yl)-phenyl)-7-(4-(trifluoromethyl)-phenyl-2-naphthoic acid]. Importantly, administration of PPTN to βENaC-Tg mice reduced neutrophil lung inflammation. These results suggest that UDP-glucose released into the airways acts as a local mediator of neutrophil inflammation.