Accumulation of Glycosphingolipids in Niemann-Pick C Disease Disrupts Endosomal Transport

Sphingolipids that contain a sphingoid base are composed of hundreds to thousands of distinct compounds, many of which serve as lipid regulators of biological functions. The global analysis of the large number of low-abundance sphingolipid molecular species has been hampered in many cases by the sphingolipid molecular species being overwhelmed by the quantity of other classes of lipid (e.g., glycerophospholipid) molecular species present, thereby imposing severe restrictions on the dynamic range of their measurement using shotgun lipidomics. Herein, we developed a facile approach in which the sphingolipids of cellular extracts were dramatically enriched by direct alkaline methanolysis of lipid extracts followed by extraction to remove the large majority of other endogenous lipid classes. Through direct infusion of the resultant enriched solution, we identified and quantitated a variety of very-low-abundance sphingolipid classes (e.g., sphingosine, psychosine, and lysosphingomyelin) and molecular species (e.g., sphingomyelin) using electrospray ionization mass spectrometry (i.e., shotgun sphingolipidomics). Accordingly, through utilization of these facile enrichment techniques, direct penetrance into the sphingolipidomes has been greatly extended, facilitating new insights into their metabolism and signaling functions in biological systems. KeywordsElectrospray ionization mass spectrometry; Shotgun lipidomics; Shotgun sphingolipidomics; Sphingolipidome; Lysosphingomyelin; Psychosine; Sphingomyelin; Sphingosine Lipidomics, the large-scale study of the pathways and networks of cellular lipids, is an emerging and rapidly expanding research field [1][2][3]. Currently, lipidomics research has been focused on identifying alterations in lipid metabolic pathways and networks induced by a disease state, a gene mutation (knockout or overexpression), a therapeutic treatment, or other perturbations. In the future, research in lipidomics will expand to include the dynamics of lipidomes, subcellular organizations of lipidomes, and interactions of lipids with lipids, proteins, and other cellular moieties. Although lipidomics has emerged as a distinct field only within the past few years [1][2][3], numerous new discoveries and/or advances have already been made [3][4][5][6][7][8][9][10][11][12]. Its essential roles in identifying the biochemical mechanisms of lipid metabolism, investigating the functions of an individual gene of interest, identifying novel biomarkers, and evaluating drug efficacy, among others, are becoming increasingly recognized.One of the major analytical platforms in current lipidomics practice is multidimensional massspectrometry (MS) 1 -based shotgun lipidomics [13][14][15]. This platform has now evolved into a mature technology that includes a series of simple steps such as multiplexed extractions, *Corresponding author. Fax: +1 314 362 1402. E-mail address: xianlin@wustl.edu (X. Han).. intrasource separation, identification of individual lipid molecular species using multidimensional MS, and quan...

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Section: Shotgun Sphingolipidomics Enables Identification and Quantifsupporting

confidence: 92%

“…The contents of sphingosine (and sphinganine) in the determined mouse brain and plasma samples are compiled in Table 2. These results are within the range of the values published previously [40,41].Similar to other choline-containing phospholipids, product ion analysis of protonated lysoSM shows a predominant fragment at m/z 184.1 (Fig. 4A).…”

supporting

confidence: 90%

Alkaline methanolysis of lipid extracts extends shotgun lipidomics analyses to the low-abundance regime of cellular sphingolipids

Jiang

Cheng

Yang

et al. 2007

Analytical Biochemistry

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“…N-Butyl deoxynojirimycin (NB-DNJ) is an inhibitor of the enzyme glucosylceramide synthetase, a key enzyme involved in the biosynthesis of gangliosides in animal cells. In NPC1 cells, some of the endosomal malfunction can be corrected by treating cells with NB-DNJ (35); however, the drug has little effect on reversing the cholesterol trafficking defect (22,35). Thus, it is unlikely that the cholesterol trafficking defects observed in NPC1 cells are due to secondary consequence of glycosphingolipid accumulation.…”

Section: Roles Of Npc1 and Npc2 In Endosomal/lysosomal Lipid Traffickingmentioning

confidence: 99%

Niemann-Pick Type C Disease and Intracellular Cholesterol Trafficking

Chang

Reid

Sugii

et al. 2005

Journal of Biological Chemistry

148

107

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“…Niemann Pick type C (NPC) disease (NPC1, MIM 257220; NPC2, MIM 607625) is an autosomal recessive neurovisceral disorder with an estimated incidence of 1:150,000 live birth and characterized by the accumulation of a broad spectrum of lipids including unesterified cholesterol, glycosphingolipids (GSLs), sphingosine and sphingomyelin within the lysosomes/late endosomes (LE) due to a defect in the intracellular lipid trafficking (Patterson et al 2001;te Vruchte et al 2004;Lloyd-Evans et al 2008).…”

Section: Introductionmentioning

confidence: 99%

Treatment of Human Fibroblasts Carrying NPC1 Missense Mutations with MG132 Leads to an Improvement of Intracellular Cholesterol Trafficking

et al. 2011

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Niemann Pick type C (NPC) disease is an autosomal recessive disorder characterized by the lysosomal/ late endosomal (LE) accumulation of unesterified cholesterol and other lipids due to a defect in the intracellular lipid trafficking. About 95% of patients present mutations in the NPC1 gene. Among the 290 mutations reported in the NPC1 gene, about 70% are missense. However, little information is available regarding the impact of missense mutations on NPC1 protein stability and function. In this study, we in vitro characterized the pathogenic effect of 7 NPC1 missense mutations. In all cases, the basal levels of mutant NPC1 expression were reduced with respect to wild type. Treatment of fibroblasts carrying NPC1 missense mutations in homo or hemizygosity, with the proteasome inhibitor MG132 or glycerol 10%, a chemical chaperone known to stabilize misfolded proteins, resulted in a significant increase of NPC1 protein levels in all cell lines, indicating that these mutants are subjected to proteasomal degradation due to protein misfolding The increment of NPC1 mutant protein induced by the proteasome inhibitor was associated with a localization of NPC1 protein within lysosomal/LE compartment. In cell lines carrying mutations p.N1156S, p.L1191F, p.V1165M, and p.I1061T, the increment of NPC1 mutant protein resulted in an improvement of the intracellular trafficking of cholesterol and GM1. These findings showed that it is possible to correct the NPC cellular phenotype by increasing the amount of endogenous NPC1 mutated protein, suggesting that at least some NPC1 mutations might be potentially rescued by small molecules-based chaperone therapy.

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Accumulation of Glycosphingolipids in Niemann-Pick C Disease Disrupts Endosomal Transport

Cited by 168 publications

References 92 publications

Alkaline methanolysis of lipid extracts extends shotgun lipidomics analyses to the low-abundance regime of cellular sphingolipids

Alkaline methanolysis of lipid extracts extends shotgun lipidomics analyses to the low-abundance regime of cellular sphingolipids

Niemann-Pick Type C Disease and Intracellular Cholesterol Trafficking

Treatment of Human Fibroblasts Carrying NPC1 Missense Mutations with MG132 Leads to an Improvement of Intracellular Cholesterol Trafficking

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