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脂多糖A诱导的小鼠对体温过低的耐受性及高反应性。

Lipid A-induced tolerance and hyperreactivity to hypothermia in mice.

作者信息

Greer G G, Rietschel E T

出版信息

Infect Immun. 1978 Feb;19(2):357-68. doi: 10.1128/iai.19.2.357-368.1978.

Abstract

Mice responded to lipopolysaccharide (LPS) with a dose-dependent, monophasic hypothermia reaching a maximum at 2 h postinjection. Degraded polysaccharide was not active; free lipid A, however, induced a similar pattern of hypothermia, indicating that the hypothermic principle of LPS was embedded within the lipid A component. The hypothermic response of mice to LPS was modified by prior exposure of the host to LPS. This altered reactivity was manifested by refractory periods (early and late tolerance), in which animals no longer responded with hypothermia, or a hyperreactive phase (hypersensitivity), in which hypothermic responses were greatly augmented upon LPS challenge. Thus, tolerance observed 24 h after a single injection of LPS (early tolerance) was followed, on further LPS challenge, by an enhanced hypothermic responses reaching a maximum on day 4. Further daily exposure of the animals to LPS eliminated hyperreactivity and led to the establishment of a late tolerance maximally expressed on day 8. Hyperreactivity could also be evoked on day 4 after a single injection of LPS. Mice pretreated with Salmonella S- and R-form LPS or free lipid A (Salmonella) demonstrated tolerance and hyperreactivity to both homologous and heterologous challenge. In addition, complete cross-tolerance was observed with S-form LPS derived from Shigella. It was concluded that the differential effects of LPS on host responses (tolerance and hyperreactivity) were due to lipid A.

摘要

小鼠对脂多糖(LPS)的反应呈剂量依赖性单相体温过低,在注射后2小时达到最大值。降解的多糖无活性;然而,游离脂质A诱导出类似的体温过低模式,表明LPS的体温过低原理存在于脂质A成分中。宿主预先接触LPS会改变小鼠对LPS的体温过低反应。这种改变的反应性表现为不应期(早期和晚期耐受性),即动物不再出现体温过低反应,或高反应期(超敏反应),即LPS刺激后体温过低反应大大增强。因此,单次注射LPS后24小时观察到的耐受性(早期耐受性),在进一步LPS刺激后,会出现增强的体温过低反应,在第4天达到最大值。动物每天进一步接触LPS可消除高反应性,并导致在第8天最大程度表达的晚期耐受性的建立。单次注射LPS后第4天也可诱发高反应性。用沙门氏菌S型和R型LPS或游离脂质A(沙门氏菌)预处理的小鼠对同源和异源刺激均表现出耐受性和高反应性。此外,观察到与志贺氏菌来源的S型LPS完全交叉耐受。得出的结论是,LPS对宿主反应(耐受性和高反应性)的不同影响是由于脂质A。

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