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首页> 外文期刊>Analytical chemistry >Comparative Glycomic Analysis of Sialyl Linkage Isomers by Sialic Acid Linkage-Specific Alkylamidation in Combination with Stable Isotope Labeling of alpha 2,3-Linked Sialic Acid Residues
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Comparative Glycomic Analysis of Sialyl Linkage Isomers by Sialic Acid Linkage-Specific Alkylamidation in Combination with Stable Isotope Labeling of alpha 2,3-Linked Sialic Acid Residues

机译:唾液酸键合特异性烷基酰胺与α2,3-连接的唾液酸残基稳定同位素标记的唾液酸键合烷基含量的比较糖分析

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摘要

Sialic acids form the terminal sugars in glycan chains on glycoproteins via alpha 2,3, alpha 2,6, or alpha 2,8 linkages, and structural isomers of sialyl linkages play various functional roles in cell recognition and other physiological processes. We recently developed a novel procedure based on sialic acid linkage-specific alkylamidation via lactone ring opening (aminolysis-SALSA). Herein, we have investigated an isotope labeling of alpha 2,3-linked sialic acid residues (iSALSA) using amine hydrochloride salts. One limitation of SALSA using amine hydrochloride salts may be solved by adding only tert-butylamine (t-BA) as an acid scavenger, and comparative and quantitative glycomic analyses can be performed using iSALSA. We also developed quantitative glycomic analysis using dual isotope-labeled glycans by derivatizing with aminooxy-functionalized tryptophanylarginine methyl ester (aoWR) and iSALSA at the reducing and nonreducing end, respectively. Furthermore, we demonstrate that the amount of alpha 2,3-linked sialoglycans in serum are altered during liver fibrosis using matrix-assisted laser desorption ionization-time-of-flight mass spectrometry (MALDI-TOF MS) and liquid chromatography MS (LC/MS) analyses. We revealed that the ratio of A3(3,6,6) to A3F(3,6,6) was gradually decreased along with liver fibrosis progression. Therefore, these glycan alterations are potential diagnostic markers of nonalcoholic steatohepatitis (NASH) fibrosis progression.
机译:唾液酸通过α2,3,α2,6或α2,8键在糖蛋白上形成糖蛋白链中的末端糖,并且SiaLyl键的结构异构体在细胞识别和其他生理过程中起各种功能作用。我们最近通过内酯环开口(Aminolysis-Salsa)基于唾液酸连杆特异性烷基酰胺进行了一种新的程序。在此,我们研究了使用盐酸胺盐的α2,3-连接的唾液酸残基(Isalsa)的同位素标记。使用盐酸胺盐的SALSA的一个限制可以仅通过添加叔丁胺(T-BA)作为酸清除剂来解决,并且可以使用ISALSA进行比较和定量糖型分析。我们还通过将双同位素标记的聚糖衍生通过用氨基氧基官能化的色氨酸碱基甲酯(Aowr)和Isalsa在还原和未加入末端进行了使用双同位素标记的聚糖进行了定量糖类分析。此外,我们证明使用基质辅助激光解吸电离 - 飞行时间质谱(MALDI-TOF MS)和液相色谱MS(LC / MS)分析。我们透露,A3(3,6,6)至A3F(3,6,6)的比例随着肝纤维化进展而逐渐降低。因此,这些聚糖改变是非酒精脂肪性炎(NASH)纤维化进展的潜在诊断标志物。

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  • 来源
    《Analytical chemistry》 |2019年第21期|共6页
  • 作者

    Hanamatsu Hisatoshi; Nishikaze Takashi; Tsumoto Hiroki; Ogawa Koji; Kobayashi Takashi; Yokota Ikuko; Morikawat Kenichi; Suda Goki; Sho Takuya; Nakai Masato; Miura Nobuaki; Higashino Kenichi; Sekiya Sadanori; Iwamoto Shinichi; Miura Yuri; Furukawa Jun-ichi; Tanaka Koichi; Sakamoto Naoya;

  • 作者单位

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Shimadzu Co Ltd Koichi Tanaka Mass Spectrometry Res Lab Kyoto 6048511 Japan;

    Tokyo Metropolitan Inst Gerontol Res Team Mech Aging Tokyo 1730015 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Shionogi &

    Co Ltd Shionogi Innovat Ctr Drug Discovery Sapporo Hokkaido 0010021 Japan;

    Hokkaido Univ Dept Adv Clin Glycobiol Fac Med Sapporo Hokkaido 0010021 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

    Niigata Univ Bioinformat Lab Grad Sch Med &

    Dent Sci Niigata 9518510 Japan;

    Shionogi &

    Co Ltd Shionogi Innovat Ctr Drug Discovery Sapporo Hokkaido 0010021 Japan;

    Shimadzu Co Ltd Koichi Tanaka Mass Spectrometry Res Lab Kyoto 6048511 Japan;

    Shimadzu Co Ltd Koichi Tanaka Mass Spectrometry Res Lab Kyoto 6048511 Japan;

    Tokyo Metropolitan Inst Gerontol Res Team Mech Aging Tokyo 1730015 Japan;

    Hokkaido Univ Dept Adv Clin Glycobiol Fac Med Sapporo Hokkaido 0010021 Japan;

    Shimadzu Co Ltd Koichi Tanaka Mass Spectrometry Res Lab Kyoto 6048511 Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido 0608638 Japan;

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