神经节苷类对脂多糖介导的细胞活化的体外和体内抑制作用。

Circulatory shock Pub Date : 1994-10-01
J J Mond, K Witherspoon, R K Yu, P Y Perera, S N Vogel
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引用次数: 0

摘要

添加纯化的GM1神经节苷对脂多糖(LPS)刺激的纯化B细胞增殖的抑制作用大于90%。在加入脂多糖120分钟后,B细胞中加入神经节苷脂仍能抑制B细胞的增殖,这表明抑制并不仅仅反映了脂多糖与神经节苷脂的直接结合。神经节苷也抑制抗ig抗体刺激的B细胞增殖,尽管抑制程度低于lps刺激反应的抑制程度。发现PMA+离子霉素联合刺激的b细胞增殖也被神经节苷类抑制,这表明其抑制活性并不反映干扰b细胞刺激与膜受体的结合。神经节苷类的抑制作用并不局限于B细胞,因为lps诱导的巨噬细胞产生TNF在体外也被抑制。体内也观察到神经节苷脂的抑制活性,注射可溶性神经节苷脂或植入含有神经节苷脂的缓释微球的小鼠体内对LPS的反应显示TNF的产生减少。植入这些缓释微丸的小鼠也免受lps诱导的死亡。因此,注射LPS+半乳糖胺后,对照组只有10%的小鼠存活,而实验组的存活率为64%。这种保护作用可能反映了神经节苷脂抑制lps介导的TNF生成的能力。该模型为研究神经节苷类在体外b细胞活化和巨噬细胞活化中的调控作用提供了基础。此外,这也为抑制LPS在体内引起的毒性作用提供了新的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inhibition of LPS-mediated cell activation in vitro and in vivo by gangliosides.

Addition of purified GM1 gangliosides inhibited lipopolysaccharide (LPS)-stimulated proliferation of purified B cells by greater than 90%. Addition of gangliosides to B cells as late as 120 min after the addition of LPS still inhibited B-cell proliferation, suggesting that inhibition did not simply reflect direct binding of LPS to gangliosides. Gangliosides also inhibited proliferation of B cells stimulated by anti-Ig antibodies, albeit to a lesser degree than inhibition of the LPS-stimulated response. The finding that B-cell proliferation stimulated by the combination of PMA+ionomycin was also inhibited by gangliosides suggests that its inhibitory activity did not reflect interference with binding of the B-cell stimuli to membrane receptors. The inhibitory effect of gangliosides was not restricted to B cells, since LPS-induced TNF production by macrophages was also inhibited in vitro. The inhibitory activity of gangliosides was also seen in vivo, and mice injected with soluble gangliosides or implanted with slow-release pellets impregnated with gangliosides showed reduced TNF production in vivo in response to LPS. Mice that were implanted with these slow-release pellets were also protected from LPS-induced lethality. Thus, while only 10% of control mice survived injection with LPS+galactosamine, the experimental group showed a 64% survival. It is likely that this protective effect reflects the ability of gangliosides to suppress LPS-mediated TNF production. This model provides a basis for studying a regulatory role for gangliosides in B-cell activation in vitro and macrophage activation in vitro and in vivo. Furthermore, it suggests new approaches to suppress the toxic effects induced by LPS in vivo.

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