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在血液与气体的界面处生成iC3。

Generation of iC3 at the interface between blood and gas.

作者信息

Nilsson Ekdahl K, Nilsson B, Pekna M, Nilsson U R

机构信息

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

出版信息

Scand J Immunol. 1992 Jan;35(1):85-91. doi: 10.1111/j.1365-3083.1992.tb02837.x.

Abstract

Earlier studies have shown that C3 can be denatured when blood comes in contact with a polystyrene surface. This study was undertaken to see if similar denaturation of C3 occurs at the gas-plasma interface which is found in all kinds of oxygenator used during cardio-pulmonary operations. An in vitro system consisting of gas bubbling through human blood, serum or plasma was used. The generation of C3a, as an indicator of complement activation, and iC3 and iC3 fragments were monitored. Both C3a and iC3/iC3 fragments levels were increased during bubbling. In contrast to the C3a level, no reduction in iC3/iC3 fragments formation was seen in the presence of EDTA, indicating that it was independent of complement activation. The rate of iC3/iC3 fragments generation was unaffected by the composition of the gas (pure oxygen, pure nitrogen or air), suggesting that the denaturation of C3 indeed occurred at the serum-gas interface. C3 and iC3/iC3 fragments were isolated from bubbled EDTA-chelated serum by PEG precipitation and chromatography on FPLC, using a Mono S column and detected by two ELISAs, specific for native C3 and iC3/iC3 fragments. After 240 min approximately 20% of the total amount of C3 consisted of intact iC3 and it was confirmed that this population bound to human erythrocytes.

摘要

早期研究表明,当血液与聚苯乙烯表面接触时,C3会发生变性。本研究旨在探究在心肺手术中使用的各种氧合器所存在的气-血浆界面处,是否会发生类似的C3变性。使用了一种体外系统,即让气体鼓泡通过人血、血清或血浆。监测了作为补体激活指标的C3a以及iC3和iC3片段的生成情况。鼓泡过程中C3a和iC3/iC3片段水平均升高。与C3a水平不同,在存在乙二胺四乙酸(EDTA)的情况下,未观察到iC3/iC3片段生成减少,这表明其与补体激活无关。iC3/iCз片段的生成速率不受气体组成(纯氧、纯氮或空气)的影响,这表明C3的变性确实发生在血清-气体界面。通过聚乙二醇(PEG)沉淀和使用Mono S柱在快速蛋白质液相色谱(FPLC)上进行层析,从鼓泡的EDTA螯合血清中分离出C3和iC3/iC3片段,并通过两种酶联免疫吸附测定法(ELISA)进行检测,这两种方法分别针对天然C3和iC3/iC3片段。240分钟后,约20%的C3总量由完整的iC3组成,并且证实这部分与人类红细胞结合。

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