控制全身炎症反应综合征和预防败血症的治疗性免疫调节方法。

New horizons (Baltimore, Md.) Pub Date : 1998-05-01
E Faist, C Kim
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引用次数: 0

摘要

在大量创伤应激的后遗症中,免疫反应性的实质性损害已被证明与临床对严重感染的易感性增加相关。创伤后免疫异常主要包括两种共存的机制:过度炎症和细胞介导的免疫反应抑制。我们的理解是,机体生存压倒性创伤的内源性能力是不足的,需要外源性支持来防止从全身性炎症反应综合征转变为细菌性败血症和感染性休克。免疫调节干预的目标应该在组织破坏后尽早开始,包括a)通过使用高剂量的多价免疫球蛋白和可溶性补体受体中和循环内毒素和外毒素来预防过度的巨噬细胞刺激;b)全球短期(
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Therapeutic immunomodulatory approaches for the control of systemic inflammatory response syndrome and the prevention of sepsis.

In the sequelae of massive traumatic stress, substantial impairment of immunologic reactivity has been demonstrated to correlate clinically with increased susceptibility to serious infection. Posttraumatic immune abnormalities consist basically of two coexistent mechanisms: Hyperinflammation and depression of cell-mediated immune responses. It is our understanding that the endogenous ability of the organism to survive overwhelming trauma is insufficient and requires exogenous support to prevent the conversion from systemic inflammatory response syndrome to bacterial sepsis and septic shock. The objectives of immunomodulatory interventions, which should be started as early as possible after tissue destruction, include a) prevention of excessive macrophage stimulation via neutralization of circulating endotoxins and exotoxins with high doses of polyvalent immunoglobulin and soluble complement receptors, b) global short-term (<72 hrs) down-regulation of inflammatory monocyte/macrophage and polymorphonuclear neutrophil activity, and c) restoration of cell-mediated immune performance to overcome posttraumatic functional paralysis. Among recent promising strategies, the use of granulocyte-macrophage colony-stimulating factor, pentoxifylline, and recombinant human interleukin-13 has been suggested, all of them predominantly down-regulating the Mphi (monocyte/macrophage) inflammatory potential. Cyclooxygenase inhibitors such as indomethacin and thymomimetic peptides can help normalize the immunoreactivity by restoring the forward-regulatory pathway of cell-mediated immunity responses. The efficacy of interferon to reduce infection and deaths in severely injured patients has been assessed in clinical trials. Still other compounds, i.e., CNI-1493, interleukin-11, tissue factor pathway inhibitors, and PGG-Glucan represent auspicious immunomodulatory approaches for control of posttraumatic or postoperative infections.

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