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用蛇毒磷脂酶A2、免疫复合物和A23187诱导人中性粒细胞内源性花生四烯酸代谢

Induction of endogenous arachidonic acid metabolism in human neutrophils with snake venom phospholipase A2, immune complexes, and A23187.

作者信息

Langholz E, Nielsen O H

机构信息

Department of Medical Gastroenterology C, Herlev Hospital, University of Copenhagen, Denmark.

出版信息

Prostaglandins Leukot Essent Fatty Acids. 1990 Mar;39(3):227-9. doi: 10.1016/0952-3278(90)90077-x.

Abstract

The stimuli responsible for eicosanoid secretion of phagocytes in chronic inflammatory disorders like rheumatoid arthritis and chronic inflammatory bowel disease are unknown. Phospholipase A2 (PLA2), found in Russelli vipera snake venom, has been proposed to be more than 100 times more potent on a molar basis than A23187 in releasing leukotriene B4 (LTB4) from porcine neutrophils. Therefore, this enzyme was investigated as a challenger of human neutrophils (PMNs) and compared with immune complexes and A23187. 1-14C-Arachidonic acid (AA) was incorporated into purified human PMNs until steady state conditions were obtained. AA release and metabolism were stimulated with either PLA2 isoenzyme of Russelli vipera, immune complexes, or A23187. The radioactive eicosanoids released were extracted and separated by thin layer chromatography, followed by autoradiography and quantitative laser densitometry. Stimulation with PLA2, immune complexes, or A23187 resulted in LTB4 formation of 0%, 1.8%, and 5.3%, respectively, of total released radioactivity. In conclusion, Russelli vipera PLA2 does not stimulate AA-release and metabolism in human PMNs, and immune complexes are weak as compared to the unphysiologic challenger A23187 in this respect.

摘要

在类风湿性关节炎和慢性炎症性肠病等慢性炎症性疾病中,负责吞噬细胞类花生酸分泌的刺激因素尚不清楚。在罗素蝰蛇毒液中发现的磷脂酶A2(PLA2),在释放猪中性粒细胞中的白三烯B4(LTB4)方面,其摩尔效力比A23187高出100倍以上。因此,对这种酶作为人类中性粒细胞(PMN)的刺激物进行了研究,并与免疫复合物和A23187进行了比较。将1-14C-花生四烯酸(AA)掺入纯化的人类PMN中,直至达到稳态条件。用罗素蝰蛇的PLA2同工酶、免疫复合物或A23187刺激AA的释放和代谢。释放出的放射性类花生酸通过薄层色谱法进行提取和分离,随后进行放射自显影和定量激光密度测定。用PLA2、免疫复合物或A23187刺激后,LTB4的形成分别占总释放放射性的0%、1.8%和5.3%。总之,罗素蝰蛇PLA2不会刺激人类PMN中AA的释放和代谢,在这方面,与非生理性刺激物A23187相比,免疫复合物的作用较弱。

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