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补体因子 C5a 和 CINC-1 在腹膜透析过程中葡萄糖转运、超滤和中性粒细胞募集中的作用。

The roles of complement factor C5a and CINC-1 in glucose transport, ultrafiltration, and neutrophil recruitment during peritoneal dialysis.

机构信息

Department of Anatomy and Cell Biology, Göteborg University, Sweden.

出版信息

Perit Dial Int. 2006 Nov-Dec;26(6):688-96.

PMID:17047237
Abstract

BACKGROUND

In a recent experimental study, we showed that low molecular weight heparin improved ultrafiltration and blocked complement activation and coagulation in a single peritoneal dialysis (PD) dwell.

OBJECTIVE

The aim of the present study was to evaluate the possible contribution of the complement factor C5a and the potential interactions between C5a, the coagulation system, and cytokines of the interleukin (IL)-8 family (cytokine-induced neutrophil chemoattractant; CINC-1).

METHODS

Nonuremic rats were exposed through an indwelling catheter to a single dose of 20 mL glucose-(2.5%) based filter-sterilized PD fluid, with or without the addition of anti-rat C5 antibody. The dwell fluid was analyzed 2 and 4 hours later concerning activation of the coagulation cascades, neutrophil recruitment, ultrafiltration volume; CINC-1, glucose, urea, and histamine concentrations; and ex vivo intraperitoneal chemotactic activity.

RESULTS

The numbers of neutrophils and levels of thrombin-antithrombin complex (TAT) and CINC-1 increased significantly during the PD dwell. C5 blockade significantly reduced the levels of TAT and increased the ultrafiltration volumes at 2 hours. Glucose concentrations were significantly positively correlated to ultrafiltration volumes.

CONCLUSIONS

Blockade of C5 leads to an increase in ultrafiltration, probably by a mechanism that involves a reduction in glucose transport. This effect may form a basis for improving PD efficiency in situations where high glucose transport limits ultrafiltration. Mechanisms connected to complement activation during PD may involve coagulation. Further studies of the intraperitoneal cascade systems under conditions of PD are indicated.

摘要

背景

在最近的一项实验研究中,我们发现低分子量肝素可改善单次腹膜透析(PD)时的超滤,并阻止补体激活和凝血。

目的

本研究旨在评估补体因子 C5a 的可能作用,以及 C5a、凝血系统和白细胞介素(IL)-8 家族细胞因子(细胞因子诱导的中性粒细胞趋化因子;CINC-1)之间的潜在相互作用。

方法

非尿毒症大鼠通过留置导管接受单次 20 mL 基于葡萄糖(2.5%)的过滤除菌 PD 液,其中添加或不添加抗大鼠 C5 抗体。2 小时和 4 小时后分析驻留液,以检测凝血级联的激活、中性粒细胞募集、超滤量;CINC-1、葡萄糖、尿素和组胺浓度;以及体外腹膜内趋化活性。

结果

在 PD 驻留期间,中性粒细胞数量和凝血酶抗凝血酶复合物(TAT)和 CINC-1 水平显著增加。C5 阻断显著降低 TAT 水平,并在 2 小时增加超滤量。葡萄糖浓度与超滤量呈显著正相关。

结论

C5 阻断导致超滤增加,可能是通过减少葡萄糖转运的机制。这一效应可能为在高葡萄糖转运限制超滤的情况下提高 PD 效率提供基础。PD 期间补体激活相关机制可能涉及凝血。建议在 PD 条件下进一步研究腹腔内级联系统。

相似文献

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The roles of complement factor C5a and CINC-1 in glucose transport, ultrafiltration, and neutrophil recruitment during peritoneal dialysis.补体因子 C5a 和 CINC-1 在腹膜透析过程中葡萄糖转运、超滤和中性粒细胞募集中的作用。
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