Intercellular Adhesion Molecule-1 Regulation In The Canine Lung After Cardiopulmonary Bypass

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Intercellular Adhesion Molecule-1 Regulation In The Canine Lung After Cardiopulmonary Bypass

William J. Dreyer, MD^a,b,c, Alan R. Burns, PhD^bc, Sharon C. Phillips, BS^a, Merry L. Lindsey, BA^c, Peggy Jackson, Gilbert L. Kukielka, MD^b,c*

Supported in part by grants HL-47163 and HL-42550 from the National Institutes of Health. During the performance of this study Alan R. Burns, PhD, was the recipient of a Fellowship from the Medical Research Council of Canada.

Received for publication June 24, 1997; revisions requested Sept. 16, 1997; revisions received Oct. 6, 1997; accepted for publication Oct. 7, 1997. Address for reprints: William J. Dreyer, MD, Pediatric Cardiology, MC 2-2280, Texas Children's Hospital, 6621 Fannin, Houston, TX 77030.

Abstract

Objective(s): Neutrophil sequestration in the lung after cardiopulmonarybypass has been shown to be dependent on the adhesion moleculeCD18. Thus we sought to determine whether endothelial expressionof intercellular adhesion molecule-1 (a ligand for CD18) inpulmonary capillaries mediates neutrophil adhesion in this setting.
Methods:Seven adult mongrel dogs underwent 90 minutes of hypothermiccardiopulmonary bypass with 60 minutes of cardioplegic arrest.After warming, dogs were reperfused for up to 9 hours and lungbiopsy specimens were obtained. Lung tissue was examined byNorthern and Western blot analysis and by immunohistologic methods.Three sham-operated dogs served as time-matched controls.
Results:Northern blots demonstrated increased expression of intercellularadhesion molecule-1 messenger ribonucleic acid within 5 minutesof cessation of bypass (or approximately 30 minutes after aorticcrossclamp release), which persisted at 9 hours of recoveryand was not present in controls. Western blots showed intercellularadhesion molecule-1 protein expression before bypass but a measurableincrease in intercellular adhesion molecule-1 protein in fourof seven dogs in the bypass group by the ninth hour of recovery.Pulmonary neutrophil accumulation 9 hours after cardiopulmonarybypass was greater in those dogs with an increased intercellularadhesion molecule-1 protein expression. Immunoelectron microscopydemonstrated the pulmonary capillary endothelium capable ofincreased intercullular adhesion molecule-1 protein expressionat the 9-hour time point.
Conclusions: Cardiopulmonary bypassresulted in intercellular adhesion molecule-1 induction in thecanine lung during recovery. An increased expression of intercellularadhesion molecule-1 protein in the lung was associated withan increased accumulation of neutrophils in affected animals.Thus intercellular adhesion molecule-1 expression may serveas a mechanism that predisposes the lungs to inflammatory cell–mediatedinjury postoperatively.

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Intercellular Adhesion Molecule-1 Regulation In The Canine Lung After Cardiopulmonary Bypass