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脂多糖和脂质A与大鼠补体的相互作用及其与内毒素毒性的关系。

Interaction of lipopolysaccharides and lipid A with complement in rats and its relation to endotoxicity.

作者信息

Freudenberg M A, Galanos C

出版信息

Infect Immun. 1978 Mar;19(3):875-82. doi: 10.1128/iai.19.3.875-882.1978.

Abstract

Uniform salt forms of endotoxic lipopolysaccharides (LPS) and free lipid A showing distinct differences in their anticomplementary activity, as well as a nontoxic LPS, are used in a new approach of studying the role of complement in endotoxin shock. The use of these defined LPS forms led to the identification of two timely, distinct depressions in complement hemolytic activity after administration of endotoxin in rats. An early depression occurred within 10 min after injection, and a late one developed more gradually, with lowest values at 6 to 9 h. The early depression represents a direct interaction of LPS with complement. It was obtained by toxic and nontoxic preparations that exhibit a high molecular weight and anticomplementary activity in vitro. The early depression was not related to the toxic properties of the LPS. The late depression was obtained only with endotoxically active LPS in lethal and 100-fold-lower concentrations, regardless of their molecular weight and of their in vitro anticomplementary activity.

摘要

具有不同抗补体活性的内毒素脂多糖(LPS)的均匀盐形式、游离脂质A以及一种无毒LPS,被用于研究补体在内毒素休克中作用的新方法。使用这些明确的LPS形式,使得在给大鼠注射内毒素后,补体溶血活性出现了两个不同时间的明显下降。早期下降在注射后10分钟内出现,后期下降则发展较为缓慢,在6至9小时达到最低值。早期下降代表LPS与补体的直接相互作用。它是通过在体外具有高分子量和抗补体活性的有毒和无毒制剂获得的。早期下降与LPS的毒性特性无关。后期下降仅在致死浓度和低100倍浓度的内毒素活性LPS中出现,无论其分子量和体外抗补体活性如何。

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