Please use this identifier to cite or link to this item: http://hdl.handle.net/2440/43772
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Type: Journal article
Title: Importance of phosphoinositide 3-kinase γ in the host defense against pneumococcal infection
Other Titles: Importance of phosphoinositide 3-kinase gamma in the host defense against pneumococcal infection
Author: Maus, U.
Backi, M.
Winter, C.
Srivastava, M.
Schwarz, M.
Ruckle, T.
Paton, J.
Briles, D.
Mack, M.
Welte, T.
Maus, R.
Bohle, R.
Seeger, W.
Rommel, C.
Hirsch, E.
Lohmeyer, J.
Preissner, K.
Citation: American Journal of Respiratory and Critical Care Medicine, 2007; 175(9):958-966
Publisher: American Thoracic Society
Issue Date: 2007
ISSN: 1073-449X
1535-4970
Statement of
Responsibility: 
Ulrich A. Maus, Myriam Backi, Christine Winter, Mrigank Srivastava, Matthias K. Schwarz, Thomas Rückle, James C. Paton, David Briles, Matthias Mack, Tobias Welte, Regina Maus, Rainer M. Bohle, Werner Seeger, Christian Rommel, Emilio Hirsch, Jürgen Lohmeyer and Klaus T. Preissner
Abstract: <h4>Rationale</h4>The pivotal role of phosphoinositide 3-kinase gamma (PI3Kgamma) in leukocyte recruitment makes it an attractive target for immunomodulatory therapy. However, interfering with PI3Kgamma signaling might increase the risk of bacterial infections in humans.<h4>Objectives</h4>We hypothesized that deletion or pharmacologic inhibition of PI3Kgamma would impair the lung inflammatory response to the prototypic gram-positive bacterial pathogen Streptococcus pneumoniae.<h4>Methods</h4>PI3Kgamma knockout (KO) and wild-type mice were infected with S. pneumoniae or challenged with the pneumococcal virulence factor pneumolysin (PLY), and inflammatory leukocyte recruitment, bacterial pathogen elimination, and resolution/repair processes were determined.<h4>Measurements and main results</h4>PI3Kgamma KO mice challenged with PLY responded with lung edema and neutrophilic alveolitis, but showed a drop in alveolar macrophages and failed to recruit exudate macrophages when compared with wild-type mice. S. pneumoniae-infected PI3Kgamma KO mice and wild-type mice pretreated with the pharmacologic inhibitor AS-605240 recruited similar numbers of neutrophils but substantially fewer exudate macrophages into their lungs than control animals. They also displayed a significantly reduced lung pneumococcal clearance and showed an impaired resolution/repair process, leading to progressive pneumococcal pneumonia.<h4>Conclusions</h4>PI3Kgamma gene deletion or pharmacologic inhibition of PI3Kgamma leads to perturbations of critical innate immune responses of the lung to challenge with S. pneumoniae. These data are of clinical relevance for the treatment of chronic inflammatory diseases where pharmacologic inhibition of PI3Kgamma signaling to attenuate effector cell recruitment may have implications for innate immune surveillance of remote organ systems.
Keywords: lung; infection; macrophage
Rights: © 2007 American Thoracic Society
RMID: 0020070749
DOI: 10.1164/rccm.200610-1533OC
Appears in Collections:Molecular and Biomedical Science publications

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