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RECEPTORS AND SIGNAL TRANSDUCTION
i proteins
1Departments of Physiology and Neuroscience, 4Pharmacology, and 5Medicine, Medical University of South Carolina, Charleston, South Carolina; 2Division of Critical Care Medicine, Cincinnati Children’s Hospital Medical Center, Cincinnati, Ohio; and 3Department of Experimental Pathology and Microbiology, Medical University of Messina, Messina, Italy
Submitted 10 August 2004 ; accepted in final form 16 March 2005
Heterotrimeric Gi proteins may play a role in lipopolysaccharide (LPS)-activated signaling through Toll-like receptor 4 (TLR4), leading to inflammatory mediator production. Although LPS is a TLR4 ligand, the gram-positive bacterium Staphylococcus aureus (SA) is a TLR2 ligand, and group B streptococci (GBS) are neither TLR2 nor TLR4 ligands but are MyD88 dependent. We hypothesized that genetic deletion of Gi proteins would alter mediator production induced by LPS and gram-positive bacterial stimulation. We examined genetic deletion of G
i2 or Gi1/3 protein in Gi2-knockout (Gi2–/–) or Gi1/3-knockout (Gi1/3–/–) mice. LPS-, heat-killed SA-, or GBS-induced mediator production in splenocytes or peritoneal macrophages (M
) was investigated. There were significant increases in LPS-, SA-, and GBS-induced production of TNF- and IFN-
in splenocytes from Gi2–/– mice compared with wild-type (WT) mice. Also, LPS-induced TNF- was increased in splenocytes from Gi1/3–/– mice. In contrast to splenocytes, LPS-, SA-, and GBS-induced TNF-, IL-10, and thromboxane B2 (TxB2) production was decreased in M harvested from Gi2–/– mice. Also, LPS-induced production of IL-10 and TxB2 was decreased in M from Gi1/3–/– mice. In subsequent in vivo studies, TNF- levels after LPS challenge were significantly greater in Gi2–/– mice than in WT mice. Also, myeloperoxidase activity, a marker of tissue neutrophil infiltration, was significantly increased in the gut and lung of LPS-treated Gi2–/– mice compared with WT mice. These data suggest that Gi proteins differentially regulate murine TLR-mediated inflammatory cytokine production in a cell-specific manner in response to both LPS and gram-positive microbial stimuli.
Gi protein-deficient mice; endotoxin; group B streptococci; Staphylococcus aureus; Toll-like receptors
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