Sphingomyelinase acts by an area-activated mechanism on the liquid-expanded phase of sphingomyelin monolayers

Tullio, Luisina De; Maggio, Bruno; Fanani, María Laura

doi:10.1194/jlr.m800127-jlr200

Cited by 32 publications

(50 citation statements)

References 31 publications

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“…A microscopy study combining DSC, fluorescence spectroscopy, and confocal fluorescence on the interaction of egg Cer with its relative egg SM showed the segregation of detergentresistant Cer-enriched domains (Sot et al 2006). In either premixed or enzyme-generated systems with bovine brain SM [mainly stearic (18:0) and lignoceric (24:0) acyl chains], Cer induces morphologically different Cer-enriched domains, depending on how the mixture was generated (Fanani et al 2002De Tullio et al 2008). Furthermore, different types of Cer-enriched domains are enzymatically formed in the presence of cholesterol, showing high solubility in cholesterol-rich membranes (Silva et al 2009;Ale et al 2012).…”

Section: Mixtures Of Ceramides With Sphingomyelins and Glycerophosphomentioning

confidence: 99%

The many faces (and phases) of ceramide and sphingomyelin II – binary mixtures

Fanani

Maggio

2017

Biophys Rev

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A rather widespread idea on the functional importance of sphingolipids in cell membranes refers to the occurrence of ordered domains enriched in sphingomyelin and ceramide that are largely assumed to exist irrespective of the type of N-acyl chain in the sphingolipid. Ceramides and sphingomyelins are the simplest kind of two-chained sphingolipids and show a variety of species, depending on the fatty acyl chain length, hydroxylation, and unsaturation. Abundant evidences have shown that variations of the N-acyl chain length in ceramides and sphingomyelins markedly affect their phase state, interfacial elasticity, surface topography, electrostatics, and miscibility, and that even the usually conceived Bcondensed^sphingolipids and many of their mixtures may exhibit liquid-like expanded states. Their lateral miscibility properties are subtlety regulated by those chemical differences. Even between ceramides with different acyl chain length, their partial miscibility is responsible for a rich twodimensional structural variety that impacts on the membrane properties at the mesoscale level. In this review, we will discuss the miscibility properties of ceramide, sphingomyelin, and glycosphingolipids that differ in their N-acyl or oligosaccharide chains. This work is a second part that accompanies a previous overview of the properties of membranes formed by pure ceramides or sphingomyelins, which is also included in this Special Issue.

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Section: Mixtures Of Ceramides With Sphingomyelins and Glycerophosphomentioning

confidence: 99%

The many faces (and phases) of ceramide and sphingomyelin II – binary mixtures

Fanani

Maggio

2017

Biophys Rev

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“…Maggio, Fanani and coworkers have reported detailed fluorescence microscopy studies of the enzymatic generation of Cer in SM monolayers in the liquid-expanded (LE) phase at the air-water interface [9,51,[54][55][56]. Their work represents one of the most comprehensive examinations of the factors that influence membrane reorganization during and after SMase activity.…”

Section: Complex Morphologies For Sphingomyelin-ceramide Monolayersmentioning

confidence: 99%

“…Several aspects of the SMase hydrolysis of SM monolayers suggest that enzymatic reaction leads to monolayer morphologies that are far from equilibrium [54][55][56]. These include the observation of different shapes and sizes for Cer-enriched domains prepared by direct mixing and enzyme action and the formation of a supersaturated Cerenriched phase during the initial lag period.…”

Section: Complex Morphologies For Sphingomyelin-ceramide Monolayersmentioning

confidence: 99%

“…Although a border-activated mechanism has been hypothesized for a number of phospholipases, other evidence suggests that some phospholipases are active over the entire fluid surface of a membrane, rather than at domain boundaries (an excellent literature summary is provided in a recent review [9]). To probe which mechanism applies to SMase hydrolysis of SM monolayers, the distribution of Alexa-488-labeled SMase was examined on SM and 9:1 SM/Cer monolayers at various stages of enzyme activity [55]. SMase was found to localize preferentially in the LE phase of both SM and SM/Cer monolayers, with no evidence for higher enzyme concentration at domain boundaries.…”

Section: Complex Morphologies For Sphingomyelin-ceramide Monolayersmentioning

confidence: 99%

“…The monolayer studies described above illustrate the complex interplay between monolayer morphology and enzyme activity and raise several mechanistic questions that have been addressed during the last two years [54][55][56]. The correlation between the formation of Cer-enriched domains and the development of full catalytic capacity at the end of the lag period was examined [56].…”

Section: Complex Morphologies For Sphingomyelin-ceramide Monolayersmentioning

confidence: 99%

See 2 more Smart Citations

Ceramide-enriched microdomains in planar membranes

Zou

Johnston

2010

Current Opinion in Colloid & Interface Science

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The many faces (and phases) of ceramide and sphingomyelin I – single lipids

Fanani

Maggio

2017

Biophys Rev

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Ceramides, the simplest kind of two-chained sphingolipids, contain a single hydroxyl group in position 1 of the sphingoid base. Sphingomyelins further contain a phosphocholine group at the OH of position 1 of ceramide. Ceramides and sphingomyelins show a variety of species depending on the fatty acyl chain length, hydroxylation, and unsaturation. Because of the relatively high transition temperature of sphingomyelin compared to lecithin and, particularly, of ceramides with 16:0-18:0 saturated chains, a widespread idea on their functional importance refers to formation of rather solid domains enriched in sphingomyelin and ceramide. Frequently, and especially in the cell biology field, these are generally (and erroneously) assumed to occur irrespective on the type of N-acyl chain in these lipids. This is because most studies indicating such condensed ordered domains employed sphingolipids with acyl chains with 16 carbons while scarce attention has been focused on the influence of the N-acyl chain on their surface properties. However, abundant evidence has shown that variations of the N-acyl chain length in ceramides and sphingomyelins markedly affect their phase state, interfacial elasticity, surface topography, electrostatics and miscibility and that, even the usually conceived "condensed" sphingolipids and many of their mixtures, may exhibit liquid-like expanded states. This review is a summarized overview of our work and of related others on some facts regarding membranes composed of single molecular species of ceramide and sphingomyelin. A second part is dedicated to discuss the miscibility properties between species of sphingolipids that differ in N-acyl and oligosaccharide chains.

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Sphingomyelinase acts by an area-activated mechanism on the liquid-expanded phase of sphingomyelin monolayers

Cited by 32 publications

References 31 publications

The many faces (and phases) of ceramide and sphingomyelin II – binary mixtures

The many faces (and phases) of ceramide and sphingomyelin II – binary mixtures

Ceramide-enriched microdomains in planar membranes

The many faces (and phases) of ceramide and sphingomyelin I – single lipids

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