AJP - Lung Cellular and Molecular Physiology, Vol 266, Issue 3 246-L254, Copyright © 1994 by American Physiological Society
Superoxide dismutase potentiates platelet-activating factor-induced injury in perfused lung
Y. C. Huang, E. S. Nozik and C. A. Piantadosi
Department of Medicine, Duke University Medical Center, Durham, North Carolina 27710.
Platelet-activating factor (PAF) causes pulmonary hypertension and lung
edema in animals and isolated perfused lungs by poorly understood
mechanisms. Because oxidative mechanisms have been implicated in
PAF-mediated cellular injury, we tested the hypothesis that superoxide
anion (O2-.) contributes to PAF-induced lung injury by determining whether
superoxide dismutase (SOD) could prevent the lung injury. Isolated rabbit
lungs were perfused with PAF (100 nM) at a dose that caused transient
hypertension and mild edema. Lungs pretreated with Cu,Zn SOD (100 U/ml) for
10 min developed persistent pulmonary hypertension and more lung edema
formation in response to PAF. Enhanced responses to PAF also were observed
in lungs perfused with 200 U/ml Cu,Zn SOD, but not with 10 or 40 U/ml Cu,Zn
SOD. The higher doses of SOD also decreased thromboxane B2 levels in the
perfusate. Potentiation of the PAF effect by Cu,Zn SOD was eliminated if
the enzyme was inactivated or if the lung was treated with an anion channel
blocker. The augmented PAF response in the presence of SOD was not altered
by catalase (200 U/ml) or by nitric oxide synthase inhibitor. The data
suggest that excessive Cu,Zn SOD enzyme activity potentiates PAF-induced
injury in perfused rabbit lung presumably by overscavenging extracellular
O2.- generated from intercellular sources. The augmented responses to PAF
are not directly attributable to increased hydrogen peroxide, nitric
oxide-related products, or thromboxane A2 production. These results suggest
the new hypothesis that a balance between O2-. production and its
metabolism determines vascular and endothelial responses to PAF.
