Secreted glucocorticoids regulate leukocyte-endothelial interactions in inflammation. A direct vital microscopic study

Leukocytes come into intimate contact with the venular endothelium as they extravasate from blood to the interstitium during inflammation. In exteriorized tissues, the number of leukocytes rolling along the vessel wall was markedly increased in adrenalectomized and metyrapone‐treated animals, relati...

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Bibliographic Details
Published in:Journal of leukocyte biology 1995-03, Vol.57 (3), p.379-386
Main Authors: Farsky, Sandra P., Sannomiya, Paulina, Garcia‐Leme, J.
Format: Article
Language:English
Subjects:
adhesion molecules
Adrenalectomy
Animals
CD11/CD18
CD18 Antigens - physiology
Cell Adhesion
Cycloheximide - pharmacology
Dactinomycin - pharmacology
Endothelium, Vascular - pathology
Glucocorticoids - physiology
Immunologic Techniques
Inflammation - pathology
Male
Metyrapone - pharmacology
Microcirculation
Mifepristone - pharmacology
Rats
Rats, Wistar
Regional Blood Flow
RU 38 486
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Summary:Leukocytes come into intimate contact with the venular endothelium as they extravasate from blood to the interstitium during inflammation. In exteriorized tissues, the number of leukocytes rolling along the vessel wall was markedly increased in adrenalectomized and metyrapone‐treated animals, relative to sham‐operated and normal animals. During the development of an acute, local inflammatory response, rollers were numerically decreased and a stronger adhesion of the cells to the endothelium, with a concomitant migration into tissues, was observed. Adhesion and migration were much more marked in adrenalectomized and metyrapone‐treated animals than in controls, suggesting that secreted glucocorticoids exert a suppressive effect on leukocyte‐endothelial interactions. The increased number of rolling leukocytes in adrenalectomized and metyrapone‐treated animals apparently resulted in more cells available to migrate into inflamed tissues. The effect appears to involve receptor occupancy and induction of gene expression because normal animals receiving the steroid antagonist RU 38 486, actinomycin D, or cydoheximide behaved as adrenalectomized or metyrapone‐treated animals. Administration to adrenalectomized animals of a monoclonal antibody to the membrane glycoprotein complex GD18 did not affect the number of rolling cells, but dramatically reduced the number of adherent or migrated leukocytes. It is suggested that secreted glucocorticoids, in addition to an effect on rolling behavior of circulating leukocytes, might also modulate the activity of the glycoprotein complex CD18 on white blood cells. The ultimate consequence is a restrictive effect on cell emigration in inflammation. J. Leukoc. Biol. 57: 379–386; 1995.
ISSN:0741-5400
1938-3673
DOI:10.1002/jlb.57.3.379