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细菌及合成脂多糖A的化学结构与生物活性

Chemical structure and biologic activity of bacterial and synthetic lipid A.

作者信息

Rietschel E T, Brade L, Brandenburg K, Flad H D, de Jong-Leuveninck J, Kawahara K, Lindner B, Loppnow H, Lüderitz T, Schade U

机构信息

Forschungsinstitut Borstel, Federal Republic of Germany.

出版信息

Rev Infect Dis. 1987 Sep-Oct;9 Suppl 5:S527-36. doi: 10.1093/clinids/9.supplement_5.s527.

Abstract

The chemical structure of the lipid A component of enterobacterial lipopolysaccharide (LPS) is now known in some detail. For example, lipid A of Escherichia coli consists of a beta(1----6)-linked D-glucosamine disaccharide that carries four (R)-3-hydroxytetradecanoyl groups in positions 2, 3, 2', and 3' and two phosphoryl residues in positions 1 and 4'. The hydroxy fatty acids at positions 2' and 3' are acylated at their 3-hydroxyl groups by dodecanoic acid and tetradecanoic acid, respectively. The hydroxyl groups in positions 4 and 6' are free, the latter serving as the attachment site for the polysaccharide component in intact LPS. On the basis of this structure, E. coli-type lipid A and partial structures thereof have been chemically synthesized (group of T. Shiba, Osaka University, Osaka, Japan) and analyzed for endotoxic activity. In all in vivo and in vitro test systems employed (including lethal toxicity, pyrogenicity, local Shwartzman reactivity, B lymphocyte mitogenicity, macrophage activation, and serologic cross-reactivity with lipid A antiserum), synthetic lipid A has activity identical to that of E. coli lipid A. These findings support the structural proposal for lipid A and prove the previous hypothesis that the endotoxic principle is embedded in lipid A.

摘要

现在已经对肠杆菌脂多糖(LPS)的脂质A成分的化学结构有了一定程度的详细了解。例如,大肠杆菌的脂质A由一个β(1→6)连接的D-葡糖胺二糖组成,该二糖在2、3、2'和3'位带有四个(R)-3-羟基十四烷酰基,在1和4'位带有两个磷酰基残基。2'和3'位的羟基脂肪酸分别在其3-羟基上被十二烷酸和十四烷酸酰化。4和6'位的羟基是游离的,后者是完整LPS中多糖成分的连接位点。基于这种结构,已经化学合成了大肠杆菌型脂质A及其部分结构(日本大阪大学的T. Shiba小组),并对其内毒素活性进行了分析。在所有使用的体内和体外测试系统中(包括致死毒性、热原性、局部施瓦茨曼反应性、B淋巴细胞促有丝分裂性、巨噬细胞活化以及与脂质A抗血清的血清学交叉反应性),合成脂质A具有与大肠杆菌脂质A相同的活性。这些发现支持了脂质A的结构提议,并证明了先前的假设,即内毒素原理存在于脂质A中。

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