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Preexposure of mouse peritoneal macrophages to lipopolysaccharide and other stimuli enhances the nitric oxide response to secondary stimuli
Authors:H. Fahmi  P. Ancuta  S. Perrier  R. Chaby
Affiliation:(1) Equipe Endotoxines, URA-1116 du C.N.R.S., Université de Paris-Sud, Bâtiment 432, F-91405 Orsay, France;(2) Laboratory of Immunology, Faculty of Science, University Sidi Mohamed Ben Abdellah, Fès, Morocco;(3) Present address: Laboratory of Immunology, Faculty of Science, University Sidi Mohamed ben Abdellah, Fès, Morocco
Abstract:The aim of this study was to compare the regulation of the production of tumor necrosis factor-agr (TNF-agr) and secondary nitric oxide (NO) in macrophages submitted to a sequence of two stimulations. Pre-exposure for 18h of mouse thioglycollate-elicited peritoneal macrophages to low doses (1–10 ng/ml) of lipopolysaccharide (LPS), in the presence or absence of serum, induces on one hand a desensitization (endotoxin tolerance) for secondary TNF-agr reponses to LPS and, on the other hand, a 4 fold increase (priming) of serondary NO responses. Preexposure to components from Gram-positive bacteria (lipoteichoic acid, peptidoglycan) and to a synthetic lipid structurally related to lipid A (compound M4), induced similar effects. In contrast to the desensitization for TNF-agr secretion, the priming for NO production was not mimicked by sodium nitroprusside, a generator of NO. The results suggest that concomitant but distinct activation pathways induced by LPS and other agents can be dissociated by serum-independent modulation processes elicited by preexposure of the cells to LPS itself, or to other stimuli.accepted by M. J. Parnham
Keywords:Lipopolysaccharide  Endotoxin tolerance  Nitric oxide  Macrophages  TNF-  /content/yk1q237258567214/xxlarge945.gif"   alt="  agr"   align="  BASELINE"   BORDER="  0"  >
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