Abstract

Bacterial infection, a complication following burn and trauma, initiates responses of the innate immune system that include rapid gene induction in myeloid (MO) and non-myeloid lineage cells. Induced genes encode cytokines, adhesive proteins and enzymes that produce proinfIammatory mediators such as oxidants or lipid metabolites. While these changes form an important part of the host defense system they unfortunately also contribute to the pathogenesis of septic shock. When Gram-negative bacteria are present it is trace amounts of endotoxin (LPS) that begins this cascade of responses. LPS-induced cell activation occurs via receptor-dependent mechanisms which involve transfer of LPS from the extracellular milieu to the cell surface via LPS binding proteins. Here our focus is on understanding how the signal from LPS is transduced in MO. In MO, a consequence of LPS binding to its receptor is triggering of kinase cascades culminating in activation of protein kinases known as MAP kinases (MAPKs). Studies during the previous grant period led to the discovery of a new member of the MAPK superfamily; we termed this enzyme p38. Subsequent work resulted in our discovery of three related but structurally distinct enzymes [MAP kinase kinases, (MKKs)] capable of activating p38. Recent evidence suggests that activation of phosphoprotein phosphatases may also be important in the LPS signal transduction cascade. It is our hypothesis that p38 activation is causally related to LPS-induced gene expression. To test this hypothesis we will perform experiments using biochemical and molecular biologic approaches to identity the predominant MKK involved in LPS-induced p38 activation, to identity substrates of p38 in order to better understand how p38 might regulate LPS-induced gene expression and to evaluate the role of phosphoprotein phosphatases in LPS-induced signalling. These studies will provide basic information that is essential to bridge the gap in our knowledge about events occurring after LPS binds to its receptor on the surface of myeloid lineage cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
5P01GM037696-15
Application #
6413614
Study Section
Project Start
2001-01-01
Project End
2002-07-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
15
Fiscal Year
2001
Total Cost
$242,857
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Tanino, Yoshinori; Chang, Mary Y; Wang, Xintao et al. (2012) Syndecan-4 regulates early neutrophil migration and pulmonary inflammation in response to lipopolysaccharide. Am J Respir Cell Mol Biol 47:196-202
Manukyan, Maria; Nalbant, Perihan; Luxen, Sylvia et al. (2009) RhoA GTPase activation by TLR2 and TLR3 ligands: connecting via Src to NF-kappa B. J Immunol 182:3522-9
Kurahashi, Kiyoyasu; Sawa, Teiji; Ota, Maria et al. (2009) Depletion of phagocytes in the reticuloendothelial system causes increased inflammation and mortality in rabbits with Pseudomonas aeruginosa pneumonia. Am J Physiol Lung Cell Mol Physiol 296:L198-209
Lu, Miao; Lin, Su-Chang; Huang, Yihua et al. (2007) XIAP induces NF-kappaB activation via the BIR1/TAB1 interaction and BIR1 dimerization. Mol Cell 26:689-702
Lombardo, Eleuterio; Alvarez-Barrientos, Alberto; Maroto, Beatriz et al. (2007) TLR4-mediated survival of macrophages is MyD88 dependent and requires TNF-alpha autocrine signalling. J Immunol 178:3731-9
da Silva Correia, J; Miranda, Y; Leonard, N et al. (2007) Regulation of Nod1-mediated signaling pathways. Cell Death Differ 14:830-9
Kang, Young Jun; Kim, Sung Ouk; Shimada, Shigeki et al. (2007) Cell surface 4-1BBL mediates sequential signaling pathways 'downstream'of TLR and is required for sustained TNF production in macrophages. Nat Immunol 8:601-9
Kravchenko, Vladimir V; Kaufmann, Gunnar F; Mathison, John C et al. (2006) N-(3-oxo-acyl)homoserine lactones signal cell activation through a mechanism distinct from the canonical pathogen-associated molecular pattern recognition receptor pathways. J Biol Chem 281:28822-30
Ruse, Monica; Knaus, Ulla G (2006) New players in TLR-mediated innate immunity: PI3K and small Rho GTPases. Immunol Res 34:33-48
Martyn, Kendra D; Frederick, Linda M; von Loehneysen, Katharina et al. (2006) Functional analysis of Nox4 reveals unique characteristics compared to other NADPH oxidases. Cell Signal 18:69-82

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