Early surfactant administration protects against lung dysfunction in a mouse model of ARDS

doi:10.1152/ajplung.00391.2002

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Am J Physiol Lung Cell Mol Physiol 284: L783-L790, 2003. First published January 17, 2003; doi:10.1152/ajplung.00391.2002
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Vol. 284, Issue 5, L783-L790, May 2003

Early surfactant administration protects against lung dysfunction in a mouse model of ARDS

Vijay P. A. Rasaiah, Jaret L. Malloy, James F. Lewis, and Ruud A. W. Veldhuizen

Departments of Physiology and Pharmacology and Medicine, Lawson Health Research Institute, University of Western Ontario, London, Ontario N6A 4V2, Canada

Sepsis can predispose the lung to insults such as mechanical ventilation (MV). It was hypothesized that treating the lungwith exogenous surfactant early in the development of sepsis willreduce the lung dysfunction associated with MV 18 h later. Miceunderwent sham or cecal ligation and perforation (CLP) surgery.Immediately after surgery, mice were either untreated or given100 mg/kg of bovine lipid extract surfactant intratracheally.Eighteen hours later, the lungs were removed and analyzed eitherimmediately or following ventilation ex vivo for 2 h by an "injurious"mode of ventilation (20 ml/kg, 0 cm positive end-expiratory pressure).In nonventilated lungs, exogenous surfactant had no impact oncompliance or IL-6 concentrations in the lungs. In the ventilatedgroups, the administered surfactant had a significant protectiveeffect on the lung dysfunction induced by MV, but only in theCLP lungs. We conclude that administration of exogenous surfactantat the time of a systemic insult can protect the lung from thedamaging effects of MV 18 hlater.

acute respiratory distress syndrome; mechanical ventilation; sepsis

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