Sphingolipid long-chain-base auxotrophs of Saccharomyces cerevisiae: genetics, physiology, and a method for their selection

Pinto, William J.; Srinivasan, Balaji; Shepherd, S; Schmidt, Anja; Dickson, Robert C.; Lester, Robert L.

doi:10.1128/jb.174.8.2565-2574.1992

Cited by 100 publications

(87 citation statements)

References 28 publications

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“…Strains were cultivated at 24, 30, or 37°C in YPD-rich medium (1% Bacto yeast extract, 2% Bacto peptone (USBiological, Swampscott, MA), 2% glucose) or in minimal medium. Cells lacking sphingolipids were cultivated in complete synthetic medium or complete complex medium as described (17). Phytosphingosine (PHS) was supplemented in 0.5% Tergitol at a concentration of 25 M. The presence of the kanMX marker was selected for by growing the cells on medium containing 200 g/ml G418 (Invitrogen).…”

Section: Methodsmentioning

confidence: 99%

Very Long-chain Fatty Acid-containing Lipids rather than Sphingolipids per se Are Required for Raft Association and Stable Surface Transport of Newly Synthesized Plasma Membrane ATPase in Yeast

Gaigg

Toulmay

Schneiter

2006

Journal of Biological Chemistry

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The proton-pumping H ؉ -ATPase, Pma1p, is an abundant and very long lived polytopic protein of the yeast plasma membrane. Pma1p constitutes a major cargo of the secretory pathway and thus serves as a model to study plasma membrane biogenesis. Pma1p associates with detergent-resistant membrane domains (lipid "rafts") already in the ER, and a lack of raft association correlates with mistargeting of the protein to the vacuole, where it is degraded. We are analyzing the role of specific lipids in membrane domain formation and have previously shown that surface transport of Pma1p is independent of newly synthesized sterols but that sphingolipids with C26 very long chain fatty acid are crucial for raft association and surface transport of Pma1p (Gaigg, B., Timischl, B., Corbino, L., and Schneiter, R. (2005) J. Biol. Chem. 280, 22515-22522). We now describe a more detailed analysis of the function that sphingolipids play in this process. Using a yeast strain in which the essential function of sphingolipids is substituted by glycerophospholipids containing C26 very long chain fatty acids, we find that sphingolipids per se are dispensable for raft association and surface delivery of Pma1p but that the C26 fatty acid is crucial. We thus conclude that the essential function of sphingolipids for membrane domain formation and stable surface delivery of Pma1p is provided by the C26 fatty acid that forms part of the yeast ceramide.

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Section: Methodsmentioning

confidence: 99%

Very Long-chain Fatty Acid-containing Lipids rather than Sphingolipids per se Are Required for Raft Association and Stable Surface Transport of Newly Synthesized Plasma Membrane ATPase in Yeast

Gaigg

Toulmay

Schneiter

2006

Journal of Biological Chemistry

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“…87,180,288 The growth defect produced by mutation of either LCB1 or LCB2 can be circumvented by adding any one of several long-chain bases to the culture medium. 203,289 In the absence of a long-chain base, the cells stop making sphingolipids and die within a few hours, even though protein, DNA and other lipid synthesis continues. 203,289 It is not known how cells take up the relatively hydrophobic long-chain bases from the culture medium.…”

Section: Sphingolipid Biosynthetic Pathway: Genes Enzymes and Phenotmentioning

confidence: 99%

“…203,289 In the absence of a long-chain base, the cells stop making sphingolipids and die within a few hours, even though protein, DNA and other lipid synthesis continues. 203,289 It is not known how cells take up the relatively hydrophobic long-chain bases from the culture medium. Other sphingolipid metabolites, such as ceramides or long-chain base phosphates and the sphingolipids containing inositol, are not taken up by cells and this property has prevented many potentially interesting experiments from being performed.…”

Section: Sphingolipid Biosynthetic Pathway: Genes Enzymes and Phenotmentioning

confidence: 99%

Biochemistry, cell biology and molecular biology of lipids ofSaccharomyces cerevisiae

Daum

Lees

Bard

et al. 1998

Yeast

573

380

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The yeast Saccharomyces cerevisiae is a powerful experimental system to study biochemical, cell biological and molecular biological aspects of lipid synthesis. Most but not all genes encoding enzymes involved in fatty acid, phospholipid, sterol or sphingolipid biosynthesis of this unicellular eukaryote have been cloned, and many gene products have been functionally characterized. Less information is available about genes and gene products governing the transport of lipids between organelles and within membranes, turnover and degradation of complex lipids, regulation of lipid biosynthesis, and linkage of lipid metabolism to other cellular processes. Here we summarize current knowledge about lipid biosynthetic pathways in S. cerevisiae and describe the characteristic features of the gene products involved. We focus on recent discoveries in these fields and address questions on the regulation of lipid synthesis, subcellular localization of lipid biosynthetic steps, cross‐talk between organelles during lipid synthesis and subcellular distribution of lipids. Finally, we discuss distinct functions of certain key lipids and their possible roles in cellular processes. © 1998 John Wiley & Sons, Ltd.

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“…Mutations in the SPT2 subunit in Saccharomyces cerevisiae and in Chinese hamster ovary cells that render the cells deficient in synthesis of sphingoid bases lead to severe growth retardation and eventual cell death unless the cells are supplemented with exogenous sphingoid bases (Dickson and Lester, 1999;Hanada, 2003;Pinto et al, 1992). Deletion of SPT2 in Drosophila leads to embryonic lethality (Dickson and Lester, 1999;Obeid et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

Sphingolipid synthesis is necessary for kinetoplast segregation and cytokinesis in Trypanosoma brucei

Fridberg

Olson

Nakayasu

et al. 2008

Journal of Cell Science

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Sphingolipids and their metabolites have been thought crucial for cell growth and cell cycle progression, membrane and protein trafficking, signal transduction, and formation of lipid rafts; however, recent studies in trypanosomes point to the dispensability of sphingolipids in some of these processes. In this study, we explore the requirements for de novo sphingolipid biosynthesis in the insect life cycle stage of the African trypanosome Trypanosoma brucei by inhibiting the enzyme serine palmitoyltransferase (SPT2) by using RNA interference or treatment with a potent SPT2 inhibitor myriocin. Mass spectrometry revealed that upon SPT2 inhibition, the parasites contained substantially reduced levels of inositolphosphorylceramide. Although phosphatidylcholine and cholesterol levels were increased to compensate for this loss, the cells were ultimately not viable. The most striking result of sphingolipid reduction in procyclic T. brucei was aberrant cytokinesis, characterized by incomplete cleavage-furrow formation, delayed kinetoplast segregation and emergence of cells with abnormal DNA content. Organelle replication continued despite sphingolipid depletion, indicating that sphingolipids act as second messengers regulating cellular proliferation and completion of cytokinesis. Distention of the mitochondrial membrane, formation of multilamellar structures within the mitochondrion and near the nucleus, accumulation of lipid bodies and, less commonly, disruption of the Golgi complex were observed after prolonged sphingolipid depletion. These findings suggest that some aspects of vesicular trafficking may be compromised. However, flagellar membrane targeting and the association of the flagellar membrane protein calflagin with detergent-resistant membranes were not affected, indicating that the vesicular trafficking defects were mild. Our studies indicate that sphingolipid biosynthesis is vital for cell cycle progression and cell survival, but not essential for the normal trafficking of flagellar membrane-associated proteins or lipid raft formation in procyclic T. brucei.

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Sphingolipid long-chain-base auxotrophs of Saccharomyces cerevisiae: genetics, physiology, and a method for their selection

Cited by 100 publications

References 28 publications

Very Long-chain Fatty Acid-containing Lipids rather than Sphingolipids per se Are Required for Raft Association and Stable Surface Transport of Newly Synthesized Plasma Membrane ATPase in Yeast

Very Long-chain Fatty Acid-containing Lipids rather than Sphingolipids per se Are Required for Raft Association and Stable Surface Transport of Newly Synthesized Plasma Membrane ATPase in Yeast

Biochemistry, cell biology and molecular biology of lipids ofSaccharomyces cerevisiae

Sphingolipid synthesis is necessary for kinetoplast segregation and cytokinesis in Trypanosoma brucei

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