ABSTRACT
BACKGROUND: Toll-like receptors (TLRs) detect endogenous ligands released after trauma and contribute to the proinflammatory response to injury. Posttraumatic mortality correlates with the extent of the immunoinflammatory response to injury that is composed of a complex regulation of innate and adaptive immune responses. Although TLRs are known to modulate innate immune responses, their role in the suppression of lymphocyte responses following traumatic tissue injury is unclear. METHODS: This study used a murine model of severe peripheral tissue injury, involving muscle crush injury and injection of fracture components, to evaluate the roles of TLR2, TLR4, and TLR9 in the early and delayed immunoinflammatory phenotype. Posttraumatic immune dysfunction was measured in our trauma model using the following parameters: ex vivo splenocyte proliferation, TH1 cytokine release, and iNOS (inducible nitric oxide synthase) induction within splenic myeloid-derived suppressor cells. Systemic inflammation and liver damage were determined by circulating interleukin 6 levels and hepatocellular injury. RESULTS: Suppression of splenocyte responses after injury was dependent on TLR4 and TLR9 signaling as was posttraumatic iNOS upregulation in splenic myeloid-derived suppressor cells. TLR2 was found to have only a partial role through contribution to inhibition of splenocyte proliferation. This study also reveals the involvement of TLR2 and TLR4 in the initial systemic inflammatory response to traumatic tissue injury; however, this response was found to be TLR9 independent. CONCLUSION: These findings demonstrate the previously unidentified role of TLR2, TLR4, and TLR9 in the T cell-associated immune dysfunction following traumatic tissue injury. Importantly, this study also illustrates that TLRs play differing and selective roles in both the initial proinflammatory response and adaptive immune response after trauma. Furthermore, results in TLR9-deficient mice establish that the upregulation of early proinflammatory markers do not always correlate with the extent of sustained immune dysfunction. This suggests potential for targeted therapies that could limit immune dysfunction through selective inhibition of receptor function following injury.
Subject(s)
Soft Tissue Injuries/physiopathology , Systemic Inflammatory Response Syndrome/physiopathology , Toll-Like Receptor 2/physiology , Toll-Like Receptor 4/physiology , Toll-Like Receptor 9/physiology , Animals , Immunity/immunology , Immunity/physiology , Interleukin-6/physiology , Liver/immunology , Liver/physiopathology , Male , Mice , Mice, Inbred C3H , Mice, Inbred C57BL , Mice, Knockout , Signal Transduction/physiology , Soft Tissue Injuries/immunology , Spleen/cytology , Spleen/physiopathology , Systemic Inflammatory Response Syndrome/immunologyABSTRACT
RATIONALE: The dexamethasone/corticotropin-releasing hormone (Dex/CRH) test is a neuroendocrine probe involving serial blood sampling of cortisol during a standardized pharmacological challenge without inducing psychological distress in humans. Some past studies in depressed patients have shown a "normalization" or decrease in cortisol response to the Dex/CRH test following successful treatment with an antidepressant. Studies in nondepressed healthy adult samples have also shown aberrant cortisol reactivity to be associated with depression risk factors. These findings prompted research into the use of the Dex/CRH test as a tool for developing antidepressant drugs. OBJECTIVES: In this study, the Dex/CRH test was evaluated with regard to its potential utility for drug development in nonclinical samples. METHODS: The Dex/CRH test was administered before and after 6 weeks of blinded treatment with either sertraline 100 mg/day or matching placebo in 22 healthy adults (13 women, nine men). RESULTS: Cortisol response to the Dex/CRH test increased following treatment with standard doses of sertraline, compared to placebo, after controlling for age and sex. CONCLUSIONS: The observed pattern of change contrasts with results from published studies in depressed patients and with our initial hypothesis.
Subject(s)
Antidepressive Agents/pharmacology , Corticotropin-Releasing Hormone , Dexamethasone , Hydrocortisone/blood , Sertraline/pharmacology , Adult , Drug Design , Female , Follow-Up Studies , Humans , Male , Middle Aged , Young AdultABSTRACT
BACKGROUND: Although timely surgical treatment of liver disease can interrupt inflammation and reduce fibrosis, the mechanisms of repair are unknown. We questioned whether these mechanisms of repair include changes in the inflammatory infiltrate and associated biological activity of matrix metalloproteinases (MMPs) 8 and 2. METHODS: Rats (n >or= 3) underwent biliary ductal suspension for 7 days followed by decompression. Livers were collected after 7 days of obstruction (d0) and after 2, 5, and 7 days of repair (d2, d5, d7, respectively), and assessed morphometrically for collagen, polymorphonuclear cells (PMNs), Kupffer cells (KCs), and inflammatory mononuclear phagocytes (MNPs). In situ zymography was performed by using fluorogenic substrates for MMP-8 and MMP-2 to spatially localize enzymatic activity. RESULTS: Cholestatic injury resulted in significantly elevated (P Subject(s)
Cholestasis/immunology
, Cholestasis/metabolism
, Liver/immunology
, Matrix Metalloproteinase 8/metabolism
, Neutrophils/immunology
, Animals
, Bilirubin/blood
, Cholestasis/surgery
, Collagen/metabolism
, Decompression, Surgical
, Liver/metabolism
, Liver Cirrhosis/immunology
, Liver Cirrhosis/metabolism
, Liver Cirrhosis/surgery
, Liver Diseases/immunology
, Liver Diseases/metabolism
, Liver Diseases/surgery
, Male
, Matrix Metalloproteinase 2/metabolism
, Neutrophils/enzymology
, Rats
, Rats, Inbred Strains
