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Infect Immun. 1980 May;28(2):373-80. doi: 10.1128/iai.28.2.373-380.1980.
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Bacterial endotoxins: chemical structure, biological activity and role in septicaemia.细菌内毒素:化学结构、生物活性及在败血症中的作用
Scand J Infect Dis Suppl. 1982;31:8-21.
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Differential determination of the 3-Deoxy-D-mannooctulosonic acid residues in lipopolysaccharides of Salmonella minnesota rough mutants.明尼苏达沙门氏菌粗糙型突变体脂多糖中3-脱氧-D-甘露辛酮糖酸残基的差异测定
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Use of mice tolerant to lipopolysaccharide to demonstrate requirement of cooperation between macrophages and lymphocytes to generate lipopolysaccharide-induced colony-stimulating factor in vivo.利用对脂多糖耐受的小鼠来证明巨噬细胞与淋巴细胞之间在体内产生脂多糖诱导的集落刺激因子时需要相互协作。
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The fate of lipopolysaccharide in rats: evidence for chemical alteration in the molecule.大鼠体内脂多糖的命运:分子化学改变的证据。
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A new method for the extraction of R lipopolysaccharides.一种提取R脂多糖的新方法。
Eur J Biochem. 1969 Jun;9(2):245-9. doi: 10.1111/j.1432-1033.1969.tb00601.x.
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The role of the liver in the production of fever and in pyrogenic tolerance.肝脏在发热产生及热原耐受性方面的作用。
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Biological activities of lipid A complexed with bovine-serum albumin.与牛血清白蛋白复合的脂多糖A的生物活性。
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10
Toxicity, clearance and distribution of endotoxin in mice as influenced by actinomycin D, cycloheximide, -amanitin and lead acetate.放线菌素D、环己酰亚胺、α-鹅膏蕈碱和醋酸铅对小鼠体内内毒素的毒性、清除及分布的影响
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通过脂多糖(LPS)预处理诱导对LPS-D-半乳糖胺致死性的耐受性是由巨噬细胞介导的。

Induction of tolerance to lipopolysaccharide (LPS)-D-galactosamine lethality by pretreatment with LPS is mediated by macrophages.

作者信息

Freudenberg M A, Galanos C

机构信息

Max-Planck-Institut für Immunbiologie, Freiburg, Federal Republic of Germany.

出版信息

Infect Immun. 1988 May;56(5):1352-7. doi: 10.1128/iai.56.5.1352-1357.1988.

DOI:10.1128/iai.56.5.1352-1357.1988
PMID:3356468
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC259829/
Abstract

In mice treated with D-galactosamine, lipopolysaccharide (LPS) exhibits enhanced toxicity (C. Galanos, M. A. Freudenberg, and W. Reutter, Proc. Natl. Acad. Sci. USA 76:5939-5943, 1979). Pretreatment of mice with LPS before D-galactosamine rendered them tolerant to the enhanced lethal effect of LPS. Tolerance was established at 1 h after LPS injection and, depending on the dose of LPS used for pretreatment, lasted for up to 48 h. With C3H/HeJ mice with acquired sensitivity to LPS (M. A. Freudenberg, D. Keppler, and C. Galanos, Infect. Immun. 51:891-895, 1986), i.e., mice that had been administered C3H/HeN macrophages, pretreatment with LPS induced tolerance only if the C3H/HeN macrophages were already present at the time of pretreatment. This indicates that, like lethality, induction of tolerance by LPS is a macrophage-mediated phenomenon. Direct interaction of LPS with macrophages is the first step in the initiation of tolerance or toxicity. C3H/HeN macrophages (2 X 10(7], incubated with minute amounts of LPS (0.5 to 0.02 microgram) in vitro and transferred subsequently to C3H/HeJ mice, induced lethality when administered together with or after D-galactosamine and tolerance when injected before D-galactosamine. Macrophages activated in vitro lost their tolerance- and lethality-inducing properties upon further incubation in LPS-free culture medium for 18 h. Such macrophages could be successfully restimulated by a new addition of LPS.

摘要

在用D-半乳糖胺处理的小鼠中,脂多糖(LPS)表现出增强的毒性(C. Galanos、M. A. Freudenberg和W. Reutter,《美国国家科学院院刊》76:5939 - 5943,1979)。在给予D-半乳糖胺之前用LPS对小鼠进行预处理,可使它们对LPS增强的致死作用产生耐受性。耐受性在LPS注射后1小时建立,并且根据用于预处理的LPS剂量,可持续长达48小时。对于对LPS获得性敏感的C3H/HeJ小鼠(M. A. Freudenberg、D. Keppler和C. Galanos,《感染与免疫》51:891 - 895,1986),即已给予C3H/HeN巨噬细胞的小鼠,只有在预处理时C3H/HeN巨噬细胞已经存在,LPS预处理才会诱导耐受性。这表明,与致死性一样,LPS诱导耐受性是一种巨噬细胞介导的现象。LPS与巨噬细胞的直接相互作用是耐受性或毒性启动的第一步。将C3H/HeN巨噬细胞(2×10⁷)与微量LPS(0.5至0.02微克)在体外孵育,随后转移到C3H/HeJ小鼠中,与D-半乳糖胺一起给药或在其之后给药时诱导致死性,在D-半乳糖胺之前注射时诱导耐受性。在体外激活的巨噬细胞在无LPS的培养基中进一步孵育18小时后失去其诱导耐受性和致死性的特性。这种巨噬细胞可以通过重新添加LPS成功地重新刺激。