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Tobias Eckle, Almut Grenz, Stefanie Laucher, Holger K. Eltzschig
Published in Volume 118, Issue 10
J Clin Invest. 2008; 118(10):3301–3315 doi:10.1172/JCI34203
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Figure 1
VILI in mice gene-targeted for individual ARs.

Previously characterized A1AR–/– (A; ref. 29), A2AAR–/– (B; ref. 30), A2BAR–/– (C), or A3AR–/– mice (D; ref. 22) or corresponding littermate controls were exposed to VILI, and survival times were determined during VILI. Mechanical ventilation was applied using pressure-controlled settings (inspiratory pressure of 35 mbar, inspired oxygen concentration 100%; respiratory rate and inspiratory/expiratory ratio were adjusted to maintain normal pH) until a cardiac standstill was observed in the surface electrocardiogram. Note the significantly attenuated survival of A2BAR–/– mice (C; P < 0.001, n = 8). Albumin concentration in the BAL fluid was determined by ELISA. For this purpose, the mice were mechanically ventilated using pressure-controlled ventilation with an inspired oxygen concentration of 100% for 180 minutes at 45 mbar. Note the significantly increased albumin concentration in the BAL fluid of A2BAR–/– mice (C; P < 0.001, n = 6).