Lidocaine reduces neutrophil recruitment by abolishing chemokine-induced arrest and transendothelial migration in septic patients

Authors/Editors

Research Areas

No matching items found.

Publication Details

Output type: Journal article

Author list: Berger C., Rossaint J., Van Aken H., Westphal M., Hahnenkamp K., Zarbock A.

Publisher: American Association of Immunologists

Publication year: 2014

Journal: The Journal of Immunology (0022-1767)

Volume number: 192

Issue number: 1

Start page: 367

End page: 376

Number of pages: 10

ISSN: 0022-1767

eISSN: 1550-6606

URL: http://api.elsevier.com/content/abstract/scopus_id:84891069094

• View in Web of Science
•  | 
• View on publisher site
•  | 
• View citing articles in Web of Science

Unpaywall Data

Open access status: bronze

Full text URL: https://www.jimmunol.org/content/jimmunol/192/1/367.full.pdf

Abstract

The inappropriate activation, positioning, and recruitment of leukocytes are implicated in the pathogenesis of multiple organ failure in sepsis. Although the local anesthetic lidocaine modulates inflammatory processes, the effects of lidocaine in sepsis are still unknown. This double-blinded, prospective, randomized clinical trial was conducted to investigate the effect of lidocaine on leukocyte recruitment in septic patients. Fourteen septic patients were randomized to receive either a placebo (n = 7) or a lidocaine (n = 7) bolus (1.5 mg/kg), followed by continuous infusion (100 mg/h for patients >70 kg or 70 mg/h for patients <70 kg) over a period of 48 h. Selectin-mediated slow rolling, chemokine-induced arrest, and transmigration were investigated by using flow chamber and transmigration assays. Lidocaine treatment abrogated chemokine-induced neutrophil arrest and significantly impaired neutrophil transmigration through endothelial cells by inhibition of the protein kinase C-θ while not affecting the selectin-mediated slow leukocyte rolling. The observed results were not attributable to changes in surface expression of adhesion molecules or selectinmediated capturing capacity, indicating a direct effect of lidocaine on signal transduction in neutrophils. These data suggest that lidocaine selectively inhibits chemokine-induced arrest and transmigration of neutrophils by inhibition of protein kinase C-θ while not affecting selectin-mediated slow rolling. These findings may implicate a possible therapeutic role for lidocaine in decreasing the inappropriate activation, positioning, and recruitment of leukocytes during sepsis. Copyright © 2013 by The American Association of Immunologists, Inc.

Keywords

No matching items found.

Documents

No matching items found.