AI Article Synopsis

  • A lethal septic shock model, known as the generalized Shwartzman reaction (GSR), was induced in mice through two LPS injections, highlighting the roles of IL-12 for priming and TNF as an effector.
  • Human studies showed that peripheral blood mononuclear cells (PBMC) from healthy adults and the elderly produced significantly more TNF when primed with IL-12 compared to PBMC without priming, suggesting an age-dependent enhancement in response.
  • The study found that while children’s PBMC produced IFN-gamma after IL-12 priming, they did not trigger a strong GSR response, indicating that age-related changes in immune cell composition, particularly NK and macrophage cells, contribute to the increased susceptibility

Article Abstract

A lethal human septic shock model, mouse generalized Shwartzman reaction (GSR), was elicited by two consecutive lippolysaccharide (LPS) injections (24 h apart) in which interferon-gamma (IFN-gamma) induced by interleukin (IL)-12 played a critical role in the priming phase, and tumor necrosis factor (TNF) was an important effector molecule in the second phase. We recently reported IL-12/LPS-induced mouse GSR age-dependently enhanced. We herein demonstrate that human peripheral blood mononuclear cells (PBMC) from healthy adults/elderly, cultured with IL-12 for 24 h and with LPS for an additional 24 h, produced a much larger amount of TNF (which increased age-dependently) than did PBMC without IL-12 priming. Whereas macrophages mainly produced TNF following LPS stimulation, macrophages and lymphocytes were necessary for a sufficient TNF production. IL-12-induced IFN-gamma up-regulated Toll-like receptor 4 (TLR-4) on macrophages of adults. Although the PBMC from children produced a substantial amount of IFN-gamma after IL-12 priming, the GSR response, with augmented TNF production and an up-regulated TLR-4 expression of macrophages, was not elicited by LPS stimulation. CD56+natural killer cells, CD56+T cells, and CD57+T cells (NK-T cells), which age-dependently increased in PBMC, produced much larger amounts of IFN-gamma after IL-12 priming than that of conventional CD56-CD57-T cells and also induced cocultured macrophages to produce TNF by subsequent LPS stimulation. The elder septic patients were consistently more susceptible to lethal shock with enhanced serum TNF levels than the adult patients. The NK cells, NK-T cells, and macrophages, which change proportionally or functionally with aging, might be involved in the enhanced GSR response/septic shock observed in elderly patients.

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Source
http://dx.doi.org/10.1189/jlb.0705396DOI Listing

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