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Synthesis and Mass Spectral Characterization of Mycobacterial Phosphatidylinositol and Its Dimannosides

机译:分枝杆菌磷脂酰肌醇及其二甘露糖苷的合成及质谱表征

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摘要

A family of naturally occurring mycobacterial phosphatidylinositol (PI) and its dimannosides (PIM2, AcPIM2, and Ac2PIM2) that all possess the predominant natural 19:0/16:0 phosphatidyl acylation pattern were prepared to study their mass spectral fragmentations. Among these, the first synthesis of a fully lipidated PIM (i.e., (16:0,18:0)(19:0/16:0)-PIM2) was achieved from (±)-1,2:4,5-diisopropylidene-d-myo-inositol in 16 steps in 3% overall yield. A key feature of the strategy was extending the utility of the p-(3,4-dimethoxyphenyl)benzyl protecting group for its use at the O-3 position of inositol to allow installation of the stearoyl residue at a late stage in the synthesis. Mass spectral studies were performed on the synthetic PIMs and compared to those reported for natural PIMs identified from a lipid extract of M. bovis BCG. These analyses confirm that fragmentation patterns can be used to identify the structures of specific PIMs from the cell wall lipid extract.
机译:准备一个自然分枝的磷脂酰肌醇(PI)及其二甘露糖苷(PIM2,AcPIM2和Ac2PIM2)家族,它们均具有主要的天然19:0/16:0磷脂酰酰化模式,以研究其质谱裂解。其中,完全脂化的PIM(即(16:0,18:0)(19:0/16:0)-PIM2)的首次合成是由(±)-1,2:4,5-二异亚丙基-d-肌醇分16步进行,总收率3%。该策略的关键特征是扩展了对-(3,4-二甲氧基苯基)苄基保护基在肌醇的O-3位置上的应用,以允许在合成的后期安装硬脂酰残基。对合成PIM进行了质谱研究,并将其与从牛分枝杆菌BCG脂质提取物中鉴定的天然PIM的报道进行了比较。这些分析证实,片段化模式可用于从细胞壁脂质提取物中鉴定特定PIM的结构。

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