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大鼠肝脏分离的质膜对内毒素的分解及产物结合的缺乏

Disaggregation of endotoxin by isolated rat liver plasma membranes and lack of product binding.

作者信息

Jones R B, Staton A J, Kiesow L A

出版信息

Infect Immun. 1974 Oct;10(4):823-30. doi: 10.1128/iai.10.4.823-830.1974.

Abstract

The interaction of bacterial endotoxin with isolated rat liver cell membranes was studied to determine the extent and nature of any binding. Serratia marcescens endotoxin was incubated with isolated rat liver plasma membranes for varying periods of time at 37 C, and this mixture was then centrifuged through a discontinous sucrose density gradient. The membranes banded primarily at the 35 to 45% sucrose interface, whether or not they had been incubated with endotoxin. The endotoxin distributed itself throughout the gradient except when incubated with membranes, in which case it failed to sediment. This membrane-induced alteration in sedimentation could be prevented by heat inactivation of the membranes, and was found to be pH, time, temperature, and concentration dependent. There was neither associated degradation of the endotoxin, as measured by molecular sieve chromatography, nor loss in toxicity, as determined in lead-sensitized rats. These observations are consistent with an enzymatic disaggregation of the endotoxin by membranes and could represent a step in the uptake of the endotoxin by the reticuloendothelial system. No significant binding of this disaggregated endotoxin to the membranes could be detected, either after gradient separation or after repeated washing. This finding strongly suggests that, at least in cells that are active in the uptake of endotoxin, membrane-endotoxin interactions may be relatively transitory in nature, and that firm adherence to such membranes may not be a central feature of endotoxin toxicity.

摘要

研究了细菌内毒素与分离的大鼠肝细胞膜的相互作用,以确定任何结合的程度和性质。将粘质沙雷氏菌内毒素与分离的大鼠肝质膜在37℃下孵育不同时间,然后将该混合物通过不连续蔗糖密度梯度离心。无论是否与内毒素孵育,膜主要在35%至45%蔗糖界面处形成条带。内毒素在整个梯度中分布,除非与膜一起孵育,在这种情况下它不会沉淀。这种膜诱导的沉降变化可以通过膜的热失活来防止,并且发现其依赖于pH、时间、温度和浓度。通过分子筛色谱法测量,内毒素既没有相关的降解,也没有如在铅致敏大鼠中所确定的毒性损失。这些观察结果与膜对内毒素的酶解聚作用一致,并且可能代表网状内皮系统摄取内毒素的一个步骤。在梯度分离后或反复洗涤后,均未检测到这种解聚的内毒素与膜有明显结合。这一发现强烈表明,至少在对内毒素摄取活跃的细胞中,膜 - 内毒素相互作用在性质上可能相对短暂,并且牢固粘附于此类膜可能不是内毒素毒性的核心特征。

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