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血小板活化因子在缺血/再灌注诱导的白细胞黏附中的作用。

Role of platelet-activating factor in ischemia/reperfusion-induced leukocyte adherence.

作者信息

Kubes P, Ibbotson G, Russell J, Wallace J L, Granger D N

机构信息

Department of Physiology, Louisiana State University Medical Center, Shreveport 71130.

出版信息

Am J Physiol. 1990 Aug;259(2 Pt 1):G300-5. doi: 10.1152/ajpgi.1990.259.2.G300.

DOI:10.1152/ajpgi.1990.259.2.G300
PMID:2166441
Abstract

The objective of this study was to determine whether platelet-activating factor (PAF) mediates the leukocyte-endothelial cell interactions elicited by ischemia/reperfusion. The rates of adherence and extravasation of leukocytes were monitored in cat mesenteric venules subjected to 60 min of ischemia (blood flow reduced to 20% of control) followed by 60 min of reperfusion. Leukocyte rolling velocity, red blood cell velocity, and vessel diameter were also measured. The experiments were performed in control (untreated) animals and in animals pretreated with one of two PAF receptor antagonists, i.e., BN 52021 or WEB 2086. The responses of venular blood flow, wall shear rate, and vessel diameter did not differ between the three groups. In the control group, 1 h of ischemia was associated with significant adherence and extravasation of leukocytes, with reperfusion greatly enhancing these responses. The rates of leukocyte adherence and extravasation during reperfusion were greatly attenuated by both PAF antagonists. Furthermore, the proportion of adherent leukocytes that ultimately extravasate during reperfusion was markedly reduced by WEB 2086. These results suggest that PAF plays an important role in mediating the adhesive interaction between circulating leukocytes and microvascular endothelium induced by ischemia/reperfusion and that the phospholipid promotes the leukocyte extravasation associated with ischemia/reperfusion.

摘要

本研究的目的是确定血小板活化因子(PAF)是否介导缺血/再灌注引发的白细胞与内皮细胞的相互作用。在猫肠系膜小静脉中监测白细胞的黏附率和渗出率,先进行60分钟的缺血(血流量降至对照的20%),然后进行60分钟的再灌注。还测量了白细胞滚动速度、红细胞速度和血管直径。实验在对照(未处理)动物以及用两种PAF受体拮抗剂之一即BN 52021或WEB 2086预处理的动物中进行。三组之间的小静脉血流量、壁剪切率和血管直径的反应没有差异。在对照组中,1小时的缺血与白细胞的显著黏附和渗出相关,再灌注大大增强了这些反应。两种PAF拮抗剂都大大减弱了再灌注期间白细胞的黏附率和渗出率。此外,WEB 2086显著降低了再灌注期间最终渗出的黏附白细胞的比例。这些结果表明,PAF在介导缺血/再灌注诱导的循环白细胞与微血管内皮之间的黏附相互作用中起重要作用,并且该磷脂促进与缺血/再灌注相关的白细胞渗出。

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