Structural determination of glycosphingolipids as lithiated adducts by electrospray ionization mass spectrometry using low-energy collisional-activated dissociation on a triple stage quadrupole instrument

被引：97

作者：

Hsu, FF ^{[1
]}

Turk, J ^{[1
]}

机构：

[1] Washington Univ, Sch Med, Dept Med, Div Endocrinol Diabet & Metab, St Louis, MO 63110 USA

来源：

JOURNAL OF THE AMERICAN SOCIETY FOR MASS SPECTROMETRY | 2001年 / 12卷 / 01期

关键词：

D O I：

10.1016/S1044-0305(00)00194-X

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

Structural characterization of glycosphingolipids as their lithiated adducts using low-energy collisional-activated dissociation (CAD) tandem mass spectrometry with electrospray ionization (ESI) is described. The tandem mass spectra contain abundant fragment ions reflecting the long chain base (LCB), fatty acid, and the sugar constituent of the molecule and permit unequivocal identification of cerebrosides, di-, trihexosyl ceramides and globosides. The major fragmentation pathways arise from loss of the sugar moiety to yield a lithiated ceramide ion, which undergoes further fragmentation to form multiple fragment ions that confirm the structures of the fatty acid and LCB. The mechanisms for the ion formation and the possible configuration of the fragment ions, resulting from CAD of the lithiated molecular ions ([M + Li](+)) of monoglycosylceramides are proposed. The mechanisms were supported by CAD and source CAD tandem mass spectra of various cerebrosides and of their analogous molecules prepared by H-D exchange. Constant neutral loss and precursor ion scannings to identify galactosylceramides with sphingosine or sphinganine LCB subclasses, and with specific N-2-hydroxyl fatty acid subclass in mixtures are also demonstrated. (C) 2001 American Society for Mass Spectrometry.

引用

页码：61 / 79

页数：19

共 28 条

[1] STRUCTURE DETERMINATION OF CERAMIDES AND NEUTRAL GLYCOSPHINGOLIPIDS BY COLLISIONAL ACTIVATION OF [M + LI]+ IONS [J].

ANN, Q ;

ADAMS, J .

JOURNAL OF THE AMERICAN SOCIETY FOR MASS SPECTROMETRY, 1992, 3 (03) :260-263

[2] STRUCTURE-SPECIFIC COLLISION-INDUCED FRAGMENTATIONS OF CERAMIDES CATIONIZED WITH ALKALI-METAL IONS [J].

ANN, QH ;

ADAMS, J .

ANALYTICAL CHEMISTRY, 1993, 65 (01) :7-13

[3] DIRECT DETERMINATION OF PHOSPHOLIPID STRUCTURES IN MICROORGANISMS BY FAST-ATOM-BOMBARDMENT TRIPLE QUADRUPOLE MASS-SPECTROMETRY [J].

COLE, MJ ;

ENKE, CG .

ANALYTICAL CHEMISTRY, 1991, 63 (10) :1032-1038

[4] TANDEM MASS-SPECTROMETRY OF GLYCOLIPIDS [J].

COSTELLO, CE ;

VATH, JE .

METHODS IN ENZYMOLOGY, 1990, 193 :738-768

[5] THE INFLUENCE OF GANGLIOSIDES ON NEURITE GROWTH AND REGENERATION [J].

DIGREGORIO, F ;

FERRARI, G ;

MARINI, P ;

SILIPRANDI, R ;

GORIO, A .

NEUROPEDIATRICS, 1984, 15 :93-96

[6] STRUCTURE ELUCIDATION OF GLYCOSPHINGOLIPIDS AND GANGLIOSIDES USING HIGH-PERFORMANCE TANDEM MASS-SPECTROMETRY [J].

DOMON, B ;

COSTELLO, CE .

BIOCHEMISTRY, 1988, 27 (05) :1534-1543

[7] A CERAMIDE ANALOG INHIBITS T-CELL PROLIFERATIVE RESPONSE THROUGH INHIBITION OF GLYCOSPHINGOLIPID SYNTHESIS AND ENHANCEMENT OF N,N-DIMETHYLSPHINGOSINE SYNTHESIS [J].

FELDINGHABERMANN, B ;

IGARASHI, Y ;

FENDERSON, BA ;

PARK, LS ;

RADIN, NS ;

INOKUCHI, J ;

STRASSMANN, G ;

HANDA, K ;

HAKOMORI, S .

BIOCHEMISTRY, 1990, 29 (26) :6314-6322

[8] GLYCOCONJUGATE EXPRESSION DURING EMBRYOGENESIS AND ITS BIOLOGICAL SIGNIFICANCE [J].

FENDERSON, BA ;

EDDY, EM ;

HAKOMORI, S .

BIOESSAYS, 1990, 12 (04) :173-179

[9]

Gorio A, 1988, Adv Neurol, V47, P523

[10]

Guittard J, 1999, RAPID COMMUN MASS SP, V13, P1838, DOI 10.1002/(SICI)1097-0231(19990930)13:18<1838::AID-RCM726>3.0.CO

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