AJP - Heart and Circulatory Physiology, Vol 256, Issue 3 751-H759, Copyright © 1989 by American Physiological Society
Cytoplasts and Mo1-deficient neutrophils pretreated with plasma and LPS induce lung injury
M. L. Wencel, M. L. Morganroth, S. O. Schoeneich, D. E. Gannon, J. Varani, R. F. Todd 3rd, U. S. Ryan and L. A. Boxer
Division of Pulmonary and Critical Care, University of Michigan, Ann Arbor 48109.
We hypothesized that neutrophil adhesion and lung injury could occur
independent of the surface receptor glycoprotein, Mo1 (C3bi receptor). We
investigated whether preincubation of human neutrophil-derived cytoplasts
(cell fragments that lack nuclei and granules and have a fixed number of
surface Mo1 receptors) with plasma and lipopolysaccharide (LPS) would
augment the cytoplasts' ability to cause lung injury when activated. We
also investigated whether preincubating normal human neutrophils treated
with anti-Mo1 antibody with plasma and LPS would increase the neutrophils'
ability to adhere and cause lung injury. Human neutrophils infused into
isolated salt-perfused rat lungs subsequently stimulated with phorbol
12-myristate 13-acetate (PMA) resulted in lung injury as assessed by the
accumulation of 125I-bovine serum albumin in the lung parenchyma. The
infusion of cytoplasts resulted in significantly less injury. Cytoplasts
preincubated in 20% human plasma and LPS caused an increase in lung injury.
Similarly, neutrophils treated with plasma, LPS, and anti-Mo1 antibody or
neutrophils congenitally deficient in the Mo1 surface receptor and treated
with plasma and LPS augmented lung injury. Plasma and LPS preincubation
also increased anti-Mo1 antibody-treated neutrophil adhesion to endothelial
cell monolayers after activation by PMA. Thus, plasma and LPS increase
adhesion and lung injury caused by neutrophils or neutrophil fragments that
share defects in Mo1 receptor expression.
