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血液透析期间的白细胞介素-1、肿瘤坏死因子及其天然拮抗剂

Interleukin-1 and tumor necrosis factor and their naturally occurring antagonists during hemodialysis.

作者信息

Dinarello C A

机构信息

Department of Medicine, Tufts University School of Medicine, Boston, Massachusetts.

出版信息

Kidney Int Suppl. 1992 Oct;38:S68-77.

PMID:1328757
Abstract

Cytokines are polypeptides which possess various biological properties affecting host defense function and response to disease. Two cytokines, interleukin-1 (IL-1) and tumor necrosis factor (TNF) induce fever, hypotension and inflammation when injected into animals or human subjects. In humans injected with either IL-1 or TNF, sleepiness, generalized myalgias and headache are commonly reported. Therefore, the production of IL-1 and TNF as a consequence of hemodialysis was hypothesized to explain, in part, the signs and symptoms of the dialysis patient. Laboratory studies confirmed that the activation of complement and the passage of microbial products from the dialysate into the blood compartment induces the synthesis of IL-1 and TNF. Although elevated production of IL-1 and TNF in the mononuclear cells and in the circulation of patients during and after hemodialysis have been reported, these levels have not been a consistent finding and are low compared to the amount of dialysis related symptoms. Recent studies, however, demonstrate that IL-1 and TNF have naturally occurring antagonists which specifically block the biological activities of these two cytokines. The IL-1 receptor antagonist blocks IL-1 binding to cells but has no IL-1 activity of itself. Soluble TNF receptors prevent TNF from binding to its cellular receptors and hence serve as anti-TNF mechanisms. These inhibitors are currently in clinical trials for sepsis where efficacy has been demonstrated; however, the IL-1 receptor antagonist (IL-1Ra) and soluble TNF receptors (sTNFR) are likely candidates for use in dialysis patients with symptomatic hypotension. Although levels of IL-1Ra and sTNFR are elevated in patients on HD, these levels reflect the host response to inflammation. It is unclear whether acute or chronic administration of IL-1Ra or sTNFR will be beneficial in treating some of the acute or chronic changes seen in dialysis patients.

摘要

细胞因子是具有多种生物学特性的多肽,可影响宿主防御功能和对疾病的反应。两种细胞因子,即白细胞介素-1(IL-1)和肿瘤坏死因子(TNF),在注射到动物或人体受试者体内时会引起发热、低血压和炎症。在注射了IL-1或TNF的人体中,常见嗜睡、全身性肌痛和头痛的报告。因此,有人推测血液透析导致的IL-1和TNF的产生部分解释了透析患者的体征和症状。实验室研究证实,补体的激活以及微生物产物从透析液进入血液腔室会诱导IL-1和TNF的合成。尽管已经报道了血液透析期间及之后患者单核细胞和循环中IL-1和TNF的产生增加,但这些水平并非一致的发现,与透析相关症状的数量相比也较低。然而,最近的研究表明,IL-1和TNF具有天然存在的拮抗剂,可特异性阻断这两种细胞因子的生物学活性。IL-1受体拮抗剂可阻断IL-1与细胞的结合,但自身不具有IL-1活性。可溶性TNF受体可阻止TNF与其细胞受体结合,因此可作为抗TNF机制。这些抑制剂目前正在脓毒症的临床试验中,已证明其有效性;然而,IL-1受体拮抗剂(IL-1Ra)和可溶性TNF受体(sTNFR)可能是用于有症状性低血压的透析患者的候选药物。尽管接受血液透析的患者体内IL-1Ra和sTNFR水平升高,但这些水平反映了宿主对炎症的反应。目前尚不清楚急性或慢性给予IL-1Ra或sTNFR是否对治疗透析患者出现的一些急性或慢性变化有益。

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