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血小板活化因子在血液透析中的作用。

Role of platelet activating factor in hemodialysis.

作者信息

Tetta C, David S, Biancone L, Canino F, Cambi V, Camussi G

机构信息

Bellco Laboratories, Bellco SpA, Mirandola (Mo), Italy.

出版信息

Kidney Int Suppl. 1993 Jan;39:S154-7.

PMID:8468919
Abstract

A complex array of inflammatory mediators are generated as a consequence of blood contact with hemodialysis (HD) membranes. Beside complement activation, other mediators are involved in cell activation, and are thought possibly to be responsible for early and long-term multiple changes in immunity infection, hypercatabolism, beta 2-microglobulin generation and hemostatic mechanisms. Previous studies from our laboratories have established platelet activating factor (PAF) as one of the mediators generated by complement-dependent or independent mechanisms of cell interaction with hemodialysis membranes. Recent studies on the production of PAF from endotoxin-primed polymorphonuclear neutrophils in a closed miniaturized circuit, and on the effect of PAF in mediating endotoxin- and cytokine-induced leukocyte adherence to HD membranes, highlight so far undescribed new roles of this mediator in biocompatibility.

摘要

血液与血液透析(HD)膜接触会产生一系列复杂的炎症介质。除补体激活外,其他介质也参与细胞激活,并且可能被认为是免疫感染、高分解代谢、β2微球蛋白生成和止血机制早期及长期多种变化的原因。我们实验室之前的研究已确定血小板活化因子(PAF)是通过细胞与血液透析膜相互作用的补体依赖性或非依赖性机制产生的介质之一。最近关于在封闭小型回路中内毒素致敏的多形核中性粒细胞产生PAF的研究,以及PAF介导内毒素和细胞因子诱导的白细胞黏附于HD膜的作用,突出了这种介质在生物相容性方面迄今未被描述的新作用。

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