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脂多糖在易感和抗性小鼠品系中的差异抗炎作用。

Differential anti-inflammatory effects of LPS in susceptible and resistant mouse strains.

作者信息

Verghese M W, Snyderman R

出版信息

J Immunol. 1981 Jul;127(1):288-93.

PMID:7240745
Abstract

Most mouse strains are highly susceptible to endotoxin (LPS) lethality and are responsive to LPS stimulation in vitro (e.g., B cell mitogenesis, macrophage activation). They are, however, capable of mounting only a small inflammatory response to LPS when it is injected i.p. The present study demonstrates that LPS is in fact a potent, anti-inflammatory agent in all of the five normally LPS susceptible strains tested. LPS was also anti-inflammatory in F1 hybrid mice from susceptible (C3HeB/FeJ) x-resistant (C3H/HeJ) parents. Anti-inflammatory effects of LPS in susceptible strains were achieved by either i.v. or i.p. treatment and were observed toward a variety of phlogistic stimuli including mitogens, C-activating substances, and nonspecific irritants. The most dramatic inhibitory effect of LPS was directed toward the accumulation of inflammatory macrophages. Kinetic studies indicated that the anti-inflammatory effect of a single dose of LPS persisted for at least 72 hr but was maximal when LPS was given simultaneously with the inflammatory stimulus. In contrast to normal mice, two mutant, LPS resistant strains (C3H/HeJ and C57BL10/ScCR) responded to increasing doses of LPS i.p. with a progressively increasing influx of inflammatory cells. In addition, in resistant strains, LPS often enhanced and never depressed the inflammatory response to other phlogistic agents. These studies demonstrate that the genetic regulation of the inflammatory responses to LPS also controls the anti-inflammatory effects of LPS. These responses may be another relevant parameter in determining strain susceptibility to LPS lethality.

摘要

大多数小鼠品系对内毒素(LPS)致死作用高度敏感,并且在体外对LPS刺激有反应(例如,B细胞有丝分裂、巨噬细胞活化)。然而,当经腹腔注射LPS时,它们对LPS仅产生微弱的炎症反应。本研究表明,事实上LPS在所有测试的五种通常对LPS敏感的品系中都是一种强效抗炎剂。LPS在来自敏感(C3HeB/FeJ)×抗性(C3H/HeJ)亲本的F1杂交小鼠中也具有抗炎作用。LPS在敏感品系中的抗炎作用通过静脉注射或腹腔注射实现,并且在针对多种促炎刺激物时都能观察到,包括有丝分裂原、补体激活物质和非特异性刺激物。LPS最显著的抑制作用针对炎症巨噬细胞的聚集。动力学研究表明,单剂量LPS的抗炎作用持续至少72小时,但当LPS与炎症刺激物同时给予时作用最大。与正常小鼠相反,两种突变的LPS抗性品系(C3H/HeJ和C57BL10/ScCR)腹腔注射递增剂量的LPS时,炎症细胞的流入量会逐渐增加。此外,在抗性品系中,LPS通常增强而从不抑制对其他促炎剂的炎症反应。这些研究表明,对LPS炎症反应的基因调控也控制着LPS的抗炎作用。这些反应可能是决定品系对LPS致死作用易感性的另一个相关参数。

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