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结核分枝杆菌脂阿拉伯甘露聚糖中阿拉伯聚糖成分的结构特征。

Structural features of the arabinan component of the lipoarabinomannan of Mycobacterium tuberculosis.

作者信息

Chatterjee D, Bozic C M, McNeil M, Brennan P J

机构信息

Department of Microbiology, Colorado State University, Fort Collins 80523.

出版信息

J Biol Chem. 1991 May 25;266(15):9652-60.

PMID:1903393
Abstract

The recent availability of pure lipoarabinomannan (LAM) from Mycobacterium spp. has resulted in its implication in host-parasite interaction, which events may be mediated by the presence of a phosphatidylinositol unit at the reducing end of LAM. Herein we address the structure of the antigenic, nonreducing end of the molecule. Through the process of 13C NMR analysis of the whole molecule and gas chromatography/mass spectrometry of alditol acetates derived from the differential per-O-alkylated lipopolysaccharide, the majority of the arabinosyl residues were recognized as furanosides. Second, through analysis of per-O-alkylated oligoarabinosyl arabinitol fragments of partially hydrolyzed LAM, it was established that the internal segments of the arabinan component consists of branched 3,5-linked alpha-D-arabinofuranosyl (Araf) units with stretches of linear 5-linked alpha-D-Araf residues attached at both branch positions, whereas the nonreducing terminal segments of LAM consist of either of the two arrangements, beta-D-Araf-(1----2)-alpha-D-Araf-(1----5)- alpha-D-Araf---- or [beta-D-Araf-(1----2)-alpha-D-Araf-(1----]2---- (3 and 5)-alpha-D-Araf----. Since this latter arrangement also characterizes the terminal segments of the peptidoglycan-bound arabinogalactan of Mycobacterium spp., we propose that mycobacteria elaborate unique terminal arabinan motifs in two distinct settings. In the case of the bound arabinogalactan, these motifs provide the nucleus for the esterified mycolic acids, entities which dominate the physicochemical features of mycobacteria and their peculiar pathogenesis. In the case of LAM, these motifs, non-mycolylated, are the dominant B-cell antigens responsible for the majority of the copious antibody response evident in most mycobacterial infections.

摘要

近期,分枝杆菌属的纯脂阿拉伯甘露聚糖(LAM)已可获取,这使得其在宿主 - 寄生虫相互作用中受到关注,这些事件可能由LAM还原端的磷脂酰肌醇单元介导。在此,我们研究该分子抗原性非还原端的结构。通过对整个分子进行¹³C NMR分析以及对差异全O - 烷基化脂多糖衍生的糖醇乙酸酯进行气相色谱/质谱分析,大多数阿拉伯糖基残基被识别为呋喃糖苷。其次,通过对部分水解的LAM的全O - 烷基化低聚阿拉伯糖基阿拉伯糖醇片段进行分析,确定阿拉伯聚糖组分的内部片段由分支的3,5 - 连接的α - D - 阿拉伯呋喃糖基(Araf)单元组成,在两个分支位置均连接有线性的5 - 连接的α - D - Araf残基链段,而LAM的非还原末端片段由两种排列方式之一组成,即β - D - Araf - (1→2) - α - D - Araf - (1→5) - α - D - Araf---- 或 [β - D - Araf - (1→2) - α - D - Araf - (1→]2---- (3和5) - α - D - Araf---- 。由于后一种排列方式也是分枝杆菌属肽聚糖结合的阿拉伯半乳聚糖末端片段的特征,我们提出分枝杆菌在两种不同情况下构建独特的末端阿拉伯聚糖基序。就结合的阿拉伯半乳聚糖而言,这些基序为酯化的分枝菌酸提供核心结构,这些物质主导了分枝杆菌及其特殊致病机制的物理化学特征。就LAM而言,这些未被分枝菌酸酰化的基序是主要的B细胞抗原,在大多数分枝杆菌感染中引发大量明显的抗体反应。

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