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Adoptive transfer of apoptotic splenocytes worsens survival, whereas adoptive transfer of necrotic splenocytes improves survival in sepsis

机译:凋亡性脾细胞的过继转移使生存恶化,而坏死性脾细胞的过继转移改善败血症的生存

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摘要

In sepsis, both necrotic and apoptotic cell death can occur. Apoptotic cells induce anergy that could impair the host response, whereas necrotic cells cause immune activation that might result in enhanced antimicrobial defenses. We determined whether adoptive transfer of apoptotic or necrotic cells impacted survival in a clinically relevant sepsis model. We also evaluated the effects of adoptive transfer of apoptotic or necrotic cells on the prototypical TH1 and TH2 cytokines IFN-γ and IL-4, respectively. C57BL6/J mice had adoptive transfer of apoptotic (irradiated) or necrotic (freeze thaw) splenocytes. Controls received saline. Apoptotic cells greatly increased mortality, whereas necrotic splenocytes markedly improved survival, P ≤ 0.05. The contrasting effects that apoptotic or necrotic cells exerted on survival were mirrored by opposite effects on splenocyte IFN-γ production with greatly decreased and increased production, respectively. Importantly, either administration of anti-IFN-γ antibodies or use of IFN-γ knockout mice prevented the survival benefit occurring with necrotic cells. This study demonstrates that the type of cell death impacts survival in a clinically relevant model and identifies a mechanism for the immune suppression that is a hallmark of sepsis. Necrotic cells (and likely apoptotic cells) exert their effects via modulation of IFN-γ
机译:在败血症中,坏死性和凋亡性细胞死亡均可发生。凋亡细胞诱导可能削弱宿主反应的无能,而坏死细胞引起免疫激活,这可能导致增强的抗微生物防御能力。我们确定凋亡或坏死细胞的过继转移是否会影响临床相关败血症模型的存活。我们还评估了凋亡或坏死细胞过继转移分别对原型TH1和TH2细胞因子IFN-γ和IL-4的影响。 C57BL6 / J小鼠过继转移了凋亡的(辐照的)或坏死的(冻融的)脾细胞。对照接受盐水。凋亡细胞大大增加了死亡率,而坏死性脾细胞显着提高了存活率,P≤0.05。凋亡或坏死细胞对存活的相反作用反映为对脾细胞IFN-γ产生的相反作用,其产生分别大大减少和增加。重要的是,施用抗IFN-γ抗体或使用IFN-γ敲除小鼠均阻止了坏死细胞的存活。这项研究表明,细胞死亡的类型会在临床相关模型中影响存活率,并确定了作为脓毒症特征的免疫抑制机制。坏死细胞(和可能的凋亡细胞)通过调节IFN-γ发挥作用

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