This assumption was important in defining different treatment str

This assumption was important in defining different treatment strategies, because most of the previous treatments using anti-inflammatory therapies were unsuccessful [57,59]. Many researchers have tried to reverse the state of immunosuppression in sepsis using IFN-γ, granulocyte colony stimulation factor (G-CSF) or granulocyte–macrophage colony stimulation factor (GM-CSF) [12,33,60]. In fact, IFN-γ administered to septic patients restored deficient HLA-DR expression, LPS-induced TNF-α production and bacterial clearance in many patients, although the effect on the immune response

is not known. In this report we have demonstrated a RU486-driven disruption of tolerance that, although using a mouse model, this website resembles those obtained by treatment with IFN-γ. In addition, in our case RU486 treatment was capable of restoring immunological competence in LPS tolerant/immunosuppressed mice. Considering that RU486 exerts a transient and reversible disruption of the regulation of tolerance/immunosuppression, but not a dismantling effect (Table 2),

this suggests that RU486 PI3K Inhibitor Library in vitro opens a window that, although transient, is central for initiation of the humoral immune response (Figs 3 and 4). In summary, in our mouse experimental model the establishment of tolerance by LPS could be inhibited by simultaneous injection of LPS with Dex, the maintenance of tolerance is dependent on GC, and overcoming endotoxin tolerance can be achieved by a competitive inhibitor of GC, RU486. These data and the preliminary observation

that RU486 can restore the primary humoral immune response in immunosuppressed mice, are important and encouraging results that deserve further investigation in a situation where the loss of immune competence can be fatal [31]. We thank Dr Susana Fink for critical reading of the manuscript, Mr Antonio Morales for technical assistance and Dr Oscar Bottasso for his help in statistical analysis. This work was supported by grants from Agencia Nacional de Promoción Científica y Tecnológica (PICT-2005-38197) acetylcholine and Fundación Alberto J. Roemmers. The authors have no conflicts of interest. “
“CD4+CD25+Foxp3+ regulatory T (TREG) cells are critical mediators of peripheral immune tolerance, and abrogation of their function provokes a variety of autoimmune and inflammatory states including inflammatory bowel disease. In this study, we investigate the functional dynamics of TREG-cell responses in a CD4+ T-cell-induced model of intestinal inflammation in αβ T-cell-deficient (TCR-β−/−) hosts to gain insights into the mechanism and cellular targets of suppression in vivo. We show that CD4+ T effector cell transfer into T-cell-deficient mice rapidly induces mucosal inflammation and colitis development, which is associated with prominent Th1 and Th17 responses.

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