Influence of Gb3 glycosphingolipids differing in their fatty acid chain on the phase behaviour of solid supported membranes: chemical syntheses and impact of Shiga toxin binding

Schütte, Ole Mathis; Ries, Annika; Orth, Alexander; Patalag, Lukas J.; Römer, Winfried; Steinem, Claudia; Werz, Daniel B.

doi:10.1039/c4sc01290a

Cited by 49 publications

(113 citation statements)

References 57 publications

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“…For lipid bilayers containing DOPC, sphingomyelin, cholesterol and Gb 3 -C24 : 0, which are phase separated at room temperature, no change in the area percentage of the l o phase was observed upon STxB binding experimentally: 13 we have shown that S-Gb 3 tends to remain phase separated in such a DOPC bilayer. Thus, SGb 3 is probably already in a phase separated state in the mixed bilayer even before STxB binds.…”

mentioning

confidence: 88%

“…Phase behaviour of such a bilayer is strongly inuenced by STxB clustering as well as the saturation levels and length of the Gb 3 fatty acyl chain. 11,13,15 Despite the important cellular roles of Gb 3 and its signicant impact on the physical behaviour of the lipid bilayers, it has not been studied by simulations before. Therefore, we use all-atom MD simulations to investigate a mixed bilayer of DOPC and Gb 3 with two different acyl chain compositions, Gb 3 -22 : 0 (Gb 3 with a saturated acyl chain with 22 carbon atoms) and Gb 3 -22 : 1 (Gb 3 with an unsaturated acyl chain with 22 carbon atoms and a trans-double bound in C 13 -C 14 ).…”

Section: 10-12mentioning

confidence: 99%

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The effects of globotriaosylceramide tail saturation level on bilayer phases

et al. 2015

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Globotriaosylceramide (Gb 3 ) is a glycosphingolipid present in the plasma membrane that is the natural receptor of the bacterial Shiga toxin. The unsaturation level of Gb 3 acyl chains has a drastic impact on lipid bilayer properties and phase behaviour, and on many Gb 3 -related cellular processes. For example:the Shiga toxin B subunit forms tubular invaginations in the presence of Gb 3 with an unsaturated acyl chain (U-Gb 3 ), while in the presence of Gb 3 with a saturated acyl chain (S-Gb 3 ) such invagination does not occur. We have used all-atom molecular dynamics simulations to investigate the effects of the Gb 3 concentration and its acyl chain saturation on the phase behaviour of a mixed bilayer of dioleoylphosphatidylcholine and Gb 3 . The simulation results show that: (1) the Gb 3 acyl chains (longer tails) from one leaflet interdigitate into the opposing leaflet and lead to significant bilayer rigidification and immobilisation of the lipid tails. S-Gb 3 can form a highly ordered, relatively immobile phase which is resistant to bending while these changes for U-Gb 3 are not significant. (2) At low concentrations of Gb 3 , U-Gb 3 and S-Gb 3 have a similar impact on the bilayer reminiscent of the effect of sphingomyelin lipids and (3) At higher Gb 3 concentrations, U-Gb 3 mixes better with dioleoylphosphatidylcholine than S-Gb 3 .Our simulations also provide the first molecular level structural model of Gb 3 in membranes.

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confidence: 88%

Section: 10-12mentioning

confidence: 99%

The effects of globotriaosylceramide tail saturation level on bilayer phases

et al. 2015

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“…They observed the existence of several laterally segregated phases, containing regions of hexagonally packed saturated hydrocarbon chains separated by cholesterol and unsaturated hydrocarbon-rich interstitial regions. Watkins [26,27]. Windschiegl et al used GUVs and planar SLBs comprising a lipid mixture of DOPC/cholesterol/Gb3 to study Shiga toxin-induced Gb3 clustering [28].…”

Section: Artificial Membrane Systems: Essential Tools For Studies On mentioning

confidence: 99%

“…This proved that sites I and II lead to high affinity receptor binding. However, site III played a role in scanning additional Gb3 receptor epitopes available for toxin binding [27].…”

Section: Shiga Toxinmentioning

confidence: 99%

Plasma membrane reorganization: A glycolipid gateway for microbes

Aigal

Claudinon

Römer

2015

Biochimica et Biophysica Acta (BBA) - Molecular Cell Research

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Ligand-receptor interactions, which represent the core for cell signaling and internalization processes are largely affected by the spatial configuration of host cell receptors. There is a growing piece of evidence that receptors are not homogeneously distributed within the plasma membrane, but are rather pre-clustered in nanodomains, or clusters are formed upon ligand binding. Pathogens have evolved many strategies to evade the host immune system and to ensure their survival by hijacking plasma membrane receptors that are most often associated with lipid rafts. In this review, we discuss the early stage molecular and physiological events that occur following ligand binding to host cell glycolipids. The ability of various biological ligands (e.g. toxins, lectins, viruses or bacteria) that bind to glycolipids to induce their own uptake into mammalian cells by creating negative membrane curvature and membrane invaginations is explored. We highlight recent trends in understanding nanoscale plasma membrane (re-)organization and present the benefits of using synthetic membrane systems. This article is part of a Special Issue entitled: Nanoscale membrane organisation and signalling.

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“…Using standard carbohydrate protecting group chemistry, 33,34 bare Gb3 was perbenzoylated, followed by anomeric deprotection and trichloroacetimidate formation. 35 In the following glycosylation reaction, globotriaosyl trichloroacetimidate ( Fig. 1(a)) and either 1,2-di-O-hexadecyl-sn-3-glycerol ( Fig.…”

Section: A Synthesis Of Gb3 Glycolipidsmentioning

confidence: 99%

Influence of length and conformation of saccharide head groups on the mechanics of glycolipid membranes: Unraveled by off-specular neutron scattering

Yamamoto

Abuillan

Burk

et al. 2015

The Journal of Chemical Physics

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The mechanical properties of multilayer stacks of Gb3 glycolipid that play key roles in metabolic disorders (Fabry disease) were determined quantitatively by using specular and off-specular neutron scattering. Because of the geometry of membrane stacks deposited on planar substrates, the scattered intensity profile was analyzed in a 2D reciprocal space map as a function of in-plane and out-of-plane scattering vector components. The two principal mechanical parameters of the membranes, namely, bending rigidity and compression modulus, can be quantified by full calculation of scattering functions with the aid of an effective cut-off radius that takes the finite sample size into consideration. The bulkier “bent” Gb3 trisaccharide group makes the membrane mechanics distinctly different from cylindrical disaccharide (lactose) head groups and shorter “bent” disaccharide (gentiobiose) head groups. The mechanical characterization of membranes enriched with complex glycolipids has high importance in understanding the mechanisms of diseases such as sphingolipidoses caused by the accumulation of non-degenerated glycosphingolipids in lysosomes or inhibition of protein synthesis triggered by the specific binding of Shiga toxin to Gb3.

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Influence of Gb3 glycosphingolipids differing in their fatty acid chain on the phase behaviour of solid supported membranes: chemical syntheses and impact of Shiga toxin binding

Cited by 49 publications

References 57 publications

The effects of globotriaosylceramide tail saturation level on bilayer phases

The effects of globotriaosylceramide tail saturation level on bilayer phases

Plasma membrane reorganization: A glycolipid gateway for microbes

Influence of length and conformation of saccharide head groups on the mechanics of glycolipid membranes: Unraveled by off-specular neutron scattering

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