4.5 Article

Detection and Structural Characterization of Ether Glycerophosphoethanolamine from Cortical Lysosomes Following Traumatic Brain Injury Using UPLC-HDMSE

期刊

PROTEOMICS
卷 19, 期 18, 页码 -

出版社

WILEY
DOI: 10.1002/pmic.201800297

关键词

data independent tandem mass spectrometry; ether lipids; glycerophosphoethanolamine; lipid structure; lysosomes; traveling wave ion mobility; traumatic brain injury; UPLC-HDMSE

资金

  1. NINDS NIH HHS [R01NS 091218, R01 NS094527, R01 NS091218] Funding Source: Medline

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The use of ultra performance liquid chromatography coupled to data independent tandem mass spectrometry with traveling wave ion mobility for detection and structural identification of ether-linked glycerophosphoethanolamine is described. The experimental design generates 4D data (chromatographic retention time, precursor accurate mass, drift time with associated calculated collisional cross-section, and time-aligned accurate mass diagnostic product ions) for each ionization mode. Confident structure identification depends on satisfying 4D data confirmation in both positive and negative ion mode. Using this methodology, a number of ether-linked glycerophosphoethanolamine lipids are structurally elucidated from mouse brain lysosomes. It is further determined that several ether-linked glycerophosphoethanolamine structures are differentially abundant between lysosomes isolated from mouse cortex following traumatic brain injury as compared to that of sham animals. The combined effort of aligning multi-dimensional mass spectrometry data with a well-defined traumatic brain injury model lays the foundation for gaining mechanistic insight in the role lysosomal membrane damage plays in neuronal cell death following brain injury.

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