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MS/MS Approach for Characterization of the Fatty Acid Distribution on Mycobacterial Phosphatidyl-myo-inositol Mannosides

机译:MS / MS方法表征分枝杆菌磷脂酰肌醇甘露糖苷上的脂肪酸分布

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摘要

Phosphatidyl-myo-inositol mannosides (PIM) are not only important structural components of the mycobacterial envelope but also are major non-peptidic antigens of the host innate and acquired immune responses. Indeed, they are ligands of TLR-2 and they activate CD1-restricted T lymphocytes. In addition, PIM constitute the basic structure of the lipidic anchor of two lipoglycans, lipomannans and lipoarabinomannans, which are important immunomodulators in the course of tuberculosis. The fatty acyl substituents present on PIM molecules play a crucial role for both their physical properties and biological activities. PIM contain four acylation sites, two on the glycerol, one on a mannose, and one on the myo-inositol units. We propose here an analytical procedure, based on mass spectrometry, to determine the structure of the fatty acids present on each of these different acylation sites. We show that the nature of the fatty acids located on both positions of glycerol can be deduced from IRMPD analysis of negative precursor ions from native PIM species, while the fatty acids located on myo-inositol and mannose units can be identified by MALDI-TOF CID MS of protonated and cationized molecular ions. Thus, the combination of MS/MS data obtained from positive and negative pseudomolecular ions generated by ESI or MALDI appears as a powerful approach for the structural characterization of the PIM acyl form structure.
机译:磷脂酰肌醇甘露糖苷(PIM)不仅是分枝杆菌包膜的重要结构成分,而且还是宿主先天和获得性免疫反应的主要非肽类抗原。实际上,它们是TLR-2的配体,并且它们激活CD1限制性T淋巴细胞。此外,PIM构成了两种脂聚糖,脂甘露聚糖和脂阿拉伯糖甘露聚糖的脂质锚的基本结构,它们是结核病过程中的重要免疫调节剂。 PIM分子上存在的脂肪酰基取代基对其物理性质和生物活性都起着至关重要的作用。 PIM包含四个酰化位点,两个在甘油上,一个在甘露糖上,一个在肌醇单元上。我们在此提出一种基于质谱的分析方法,以确定存在于这些不同酰化位点中每一个上的脂肪酸的结构。我们表明,可以从天然PIM物种的负前体离子的IRMPD分析中推断出位于甘油两个位置上的脂肪酸的性质,而可以通过MALDI-TOF CID识别位于肌醇和甘露糖单元上的脂肪酸质子化和阳离子化的分子离子的质谱。因此,从由ESI或MALDI生成的正负假分子离子获得的MS / MS数据组合似乎是对PIM酰基形式结构进行结构表征的有力方法。

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