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作为体外循环回路模型的管道环:在体外模型中,生物材料和气血相界面均可诱导补体激活。

Tubing loops as a model for cardiopulmonary bypass circuits: both the biomaterial and the blood-gas phase interfaces induce complement activation in an in vitro model.

作者信息

Gong J, Larsson R, Ekdahl K N, Mollnes T E, Nilsson U, Nilsson B

机构信息

Department of Clinical Immunology and Transfusion Medicine, University Hospital, Uppsala, Sweden.

出版信息

J Clin Immunol. 1996 Jul;16(4):222-9. doi: 10.1007/BF01541228.

Abstract

We describe here a model for the study of blood/surface and blood/air interaction as encountered in cardiopulmonary bypass (CPB) circuits. Polyethylene tubing was filled with serum or blood and closed end to end into loops whereby the volume of the remaining air bubble was inversely varied with respect to that of the fluid. The loops were rotated vertically in a water bath at 37 degrees C. The profiles of C3a, iC3, and TCC generation were similar to those observed at surgery, involving CPB. Soluble heparin and heparan sulfate inhibited both C3a and TCC formation, but surface-conjugated heparin had only a minor effect. Binding of C3 and/or C3 fragments to the heparin surface was much reduced compared to the amine matrix to which heparin was linked, but compared with the polyethylene surface the effect was less pronounced. These data suggest that, in addition to the biomaterial surface, the blood-gas interface seems to play an important role in the activation of complement and that this activation is inhibitable by high concentrations of soluble glucose aminoglycans.

摘要

我们在此描述一种用于研究体外循环(CPB)回路中血液/表面及血液/空气相互作用的模型。将聚乙烯管充满血清或血液,并首尾封闭形成环路,其中剩余气泡的体积与流体体积呈反比变化。这些环路在37℃的水浴中垂直旋转。C3a、iC3和末端补体复合物(TCC)的生成情况与CPB手术中观察到的相似。可溶性肝素和硫酸乙酰肝素抑制C3a和TCC的形成,但表面结合的肝素仅有轻微作用。与肝素连接的胺基质相比,C3和/或C3片段与肝素表面的结合显著减少,但与聚乙烯表面相比,这种作用不太明显。这些数据表明,除生物材料表面外,血气界面似乎在补体激活中起重要作用,且这种激活可被高浓度的可溶性葡萄糖胺聚糖抑制。

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