Article date: November 2006
By: S H Slofstra, A P Groot, N A Maris, P H Reitsma, H ten Cate, C A Spek in Volume 149, Issue 6, pages 740-746
Background and purpose:
Intravenous administration of recombinant human activated protein C (rhAPC) is known to reduce lipopolysaccharide (LPS)‐induced pulmonary inflammation by attenuating neutrophil chemotaxis towards the alveolar compartment. Ideally, one would administer rhAPC in pulmonary inflammation at the site of infection to minimize the risk of systemic bleeding complications. In this study, we therefore assessed the effect of inhaled rhAPC in a murine model of acute lung injury.
Experimental approach:
Mice were exposed to LPS (0.5 mg kg‐1: intranasally) to induce acute lung injury. 30 minutes before and 3 hours after LPS exposure mice were subjected to vehicle or rhAPC inhalation (25 or 100 μg per mouse in each nebulization). In order to establish whether rhAPC inhalation affects neutrophil recruitment, neutrophil migration was determined in vitro using a trans‐well migration assay.
Key results:
rhAPC inhalation dose‐dependently decreased LPS‐induced coagulation and inflammation markers in bronchoalveolar lavage fluid (BALF), reduced protein leakage into the alveolar space and improved lung function. In contrast, rhAPC did not prevent LPS‐induced neutrophil recruitment into the alveolar space.
Conclusions and Implications:
rhAPC inhalation significantly diminished LPS‐induced pulmonary inflammation. The benefit of inhaled rhAPC appeared not to involve attenuation of neutrophil recruitment, in contrast to its effects after intravenous administration.
DOI: 10.1038/sj.bjp.0706915
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