Movatterモバイル変換

[0]ホーム
URL:

Wikipedia

Sphingolipid

(Redirected fromSphingolipids)
This articleneeds additional citations forverification. Please helpimprove this article byadding citations to reliable sources. Unsourced material may be challenged and removed.
Find sources: "Sphingolipid" – news ·newspapers ·books ·scholar ·JSTOR(January 2023) (Learn how and when to remove this message)

Sphingolipids are a class oflipids containing a backbone of sphingoid bases, which are a set ofaliphaticaminoalcohols that includessphingosine. They were discovered in brain extracts in the 1870s and were named after the mythologicalsphinx because of their enigmatic nature.[1][2] These compounds play important roles insignal transduction andcell recognition.[3]Sphingolipidoses, or disorders of sphingolipid metabolism, have particular impact onneural tissue. A sphingolipid with a terminal hydroxyl group is aceramide. Other common groups bonded to the terminal oxygen atom includephosphocholine, yielding asphingomyelin, and various sugarmonomers ordimers, yieldingcerebrosides andglobosides, respectively. Cerebrosides and globosides are collectively known asglycosphingolipids.

General structures of sphingolipids

Structure

edit

The long-chain bases, sometimes simply known as sphingoid bases, are the first non-transient products ofde novo sphingolipid synthesis in both yeast and mammals. These compounds, specifically known asphytosphingosine anddihydrosphingosine (also known as sphinganine,[4] although this term is less common), are mainly C18 compounds, with somewhat lower levels of C20 bases.[5] Ceramides and glycosphingolipids areN-acyl derivatives of these compounds.[6]

The sphingosine backbone is O-linked to a (usually) charged head group such asethanolamine,serine, orcholine.[citation needed]

The backbone is also amide-linked to anacyl group, such as afatty acid.[citation needed]

Types

edit

Simple sphingolipids, which include the sphingoid bases and ceramides, make up the early products of the sphingolipid synthetic pathways.

  • Sphingoid bases are the fundamental building blocks of all sphingolipids. The main mammalian sphingoid bases are dihydrosphingosine and sphingosine, while dihydrosphingosine and phytosphingosine are the principal sphingoid bases in yeast.[7][8] Sphingosine, dihydrosphingosine, and phytosphingosine may be phosphorylated.
  • Ceramides, as a general class, areN-acylated sphingoid bases lacking additional head groups.
    • Dihydroceramide is produced byN-acylation of dihydrosphingosine. Dihydroceramide is found in both yeast and mammalian systems.
    • Ceramide is produced in mammalian systems by desaturation of dihydroceramide by dihydroceramide desaturase 1 (DES1). This highly bioactive molecule may also be phosphorylated to formceramide-1-phosphate.
    • Phytoceramide is produced in yeast by hydroxylation of dihydroceramide at C-4.

Complex sphingolipids may be formed by addition of head groups to ceramide or phytoceramide:

Mammalian sphingolipid metabolism

edit

De novo sphingolipid synthesis begins with formation of 3-keto-dihydrosphingosine byserine palmitoyltransferase.[9] The preferred substrates for this reaction arepalmitoyl-CoA andserine. However, studies have demonstrated that serine palmitoyltransferase has some activity toward other species offatty acyl-CoA[10] and alternativeamino acids,[11] and the diversity of sphingoid bases has recently been reviewed.[12] Next, 3-keto-dihydrosphingosine is reduced to form dihydrosphingosine. Dihydrosphingosine is acylated by one of six (dihydro)-ceramide synthase,CerS - originally termed LASS - to form dihydroceramide.[13] The six CerS enzymes have different specificity foracyl-CoA substrates, resulting in the generation of dihydroceramides with differing chain lengths (ranging from C14-C26). Dihydroceramides are then desaturated to form ceramide.[14]

 
Metabolic pathways of various forms of sphingolipids.Sphingolipidoses are labeled at corresponding stages that are deficient.

De novo generatedceramide is the central hub of the sphingolipid network and subsequently has several fates. It may be phosphorylated byceramide kinase to form ceramide-1-phosphate. Alternatively, it may be glycosylated byglucosylceramide synthase orgalactosylceramide synthase. Additionally, it can be converted tosphingomyelin by the addition of aphosphorylcholine headgroup bysphingomyelin synthase.Diacylglycerol is generated by this process. Finally, ceramide may be broken down by aceramidase to formsphingosine.Sphingosine may be phosphorylated to form sphingosine-1-phosphate. This may be dephosphorylated to reform sphingosine.[15]

Breakdown pathways allow the reversion of these metabolites to ceramide. The complex glycosphingolipids are hydrolyzed to glucosylceramide and galactosylceramide. These lipids are then hydrolyzed by beta-glucosidases and beta-galactosidases to regenerate ceramide. Similarly, sphingomyelin may be broken down by sphingomyelinase to form ceramide.[citation needed]

The only route by which sphingolipids are converted to non-sphingolipids is through sphingosine-1-phosphate lyase. This forms ethanolamine phosphate and hexadecenal.[16]

Functions of mammalian sphingolipids

edit

Sphingolipids are commonly believed to protect the cell surface against harmful environmental factors by forming a mechanically stable and chemically resistant outer leaflet of theplasma membranelipid bilayer. Certain complexglycosphingolipids were found to be involved in specific functions, such ascell recognition and signaling. Cell recognition depends mainly on the physical properties of the sphingolipids, whereas signaling involves specific interactions of the glycan structures of glycosphingolipids with similar lipids present on neighboring cells or withproteins.[citation needed]

Recently, simple sphingolipidmetabolites, such as ceramide andsphingosine-1-phosphate, have been shown to be important mediators in the signaling cascades involved inapoptosis,proliferation, stress responses,necrosis,inflammation,autophagy,senescence, anddifferentiation.[17][18][19][20][21] Ceramide-based lipids self-aggregate incell membranes and form separatephases less fluid than the bulk phospholipids. These sphingolipid-based microdomains, or "lipid rafts" were originally proposed to sort membrane proteins along the cellular pathways of membrane transport. At present, most research focuses on the organizing function during signal transduction.[22]

Sphingolipids are synthesized in a pathway that begins in theER and is completed in theGolgi apparatus, but these lipids are enriched in theplasma membrane and inendosomes, where they perform many of their functions.[23] Transport occurs via vesicles and monomeric transport in thecytosol. Sphingolipids are virtually absent frommitochondria and theER, but constitute a 20-35 molar fraction of plasma membrane lipids.[24]

In experimental animals, feeding sphingolipids inhibitscolon carcinogenesis, reducesLDL cholesterol and elevatesHDL cholesterol.[25]

Other sphingolipids

edit

Sphingolipids are universal ineukaryotes but are rare inbacteria andarchaea, meaning that they are evolutionally very old. Bacteria that do produce sphingolipids are found in some members of thesuperphylumFCB group (Sphingobacteria), particularly familySphingomonadaceae, some members of theBdellovibrionota, and some members of theMyxococcota.[26]

Yeast sphingolipids

edit

Because of the incredible complexity of mammalian systems, yeast are often used as amodel organism for working out new pathways. These single-celled organisms are often more genetically tractable than mammalian cells, and strain libraries are available to supply strains harboring almost any non-lethalopen reading frame single deletion. The two most commonly used yeasts areSaccharomyces cerevisiae andSchizosaccharomyces pombe, although research is also done in the pathogenic yeastCandida albicans.[citation needed]

In addition to the important structural functions of complex sphingolipids (inositol phosphorylceramide and its mannosylated derivatives), the sphingoid basesphytosphingosine and dihydrosphingosine (sphinganine) play vital signaling roles inS. cerevisiae. These effects include regulation ofendocytosis, ubiquitin-dependentproteolysis (and, thus, regulation of nutrient uptake[27]),cytoskeletal dynamics, thecell cycle,translation, posttranslational protein modification, and the heat stress response.[28] Additionally, modulation of sphingolipid metabolism byphosphatidylinositol (4,5)-bisphosphate signalingvia Slm1p and Slm2p andcalcineurin has recently been described.[29] Additionally, a substrate-level interaction has been shown between complex sphingolipid synthesis and cycling ofphosphatidylinositol 4-phosphate by the phosphatidylinositol kinase Stt4p and the lipid phosphatase Sac1p.[30]

Plant sphingolipids

edit

Higher plants contain a wider variety of sphingolipids than animals and fungi.[citation needed]

Disorders

edit
Main article:Sphingolipidoses

There are several disorders of sphingolipid metabolism, known assphingolipidoses. The main members of this group areNiemann-Pick disease,Fabry disease,Krabbe disease,Gaucher disease,Tay–Sachs disease andMetachromatic leukodystrophy. They are generally inherited in anautosomal recessive fashion, but notablyFabry disease isX-linked. Taken together, sphingolipidoses have anincidence of approximately 1 in 10,000, but substantially more in certain populations such asAshkenazi Jews.Enzyme replacement therapy is available to treat mainlyFabry disease andGaucher disease, and people with these types of sphingolipidoses may live well into adulthood. The other types are generally fatal by age 1 to 5 years for infantile forms, but progression may be mild for juvenile- or adult-onset forms.[citation needed]

Sphingolipids have also been implicated with the frataxin protein (Fxn), the deficiency of which is associated withFriedreich's ataxia (FRDA). Loss of Fxn in the nervous system in mice also activates an iron/sphingolipid/PDK1/Mef2 pathway, indicating that the mechanism is evolutionarily conserved. Furthermore, sphingolipid levels and PDK1 activity are also increased in hearts of FRDA patients, suggesting that a similar pathway is affected in FRDA.[31] Other research has demonstrated that iron accumulation in the nervous systems of flies enhances the synthesis of sphingolipids, which in turn activates 3-phosphoinositide dependent protein kinase-1 (Pdk1) and myocyte enhancer factor-2 (Mef2) to trigger neurodegeneration of adult photoreceptors.[32]

Sphingolipids play a key role in neuronal survival in Parkinson's Disease (PD) and their catabolic pathway alteration in the brain is partly represented in cerebrospinal fluid and blood tissues (Table1) and have the diagnostic potential.[33]

Additional images

edit

See also

edit

References

edit
  1. ^Chun J, Hartung HP (2010)."Mechanism of action of oral fingolimod (FTY720) in multiple sclerosis".Clinical Neuropharmacology.33 (2):91–101.doi:10.1097/wnf.0b013e3181cbf825.PMC 2859693.PMID 20061941.
  2. ^Schnaar, Ronald L.; Sandhoff, Roger; Tiemeyer, Michael; Kinoshita, Taroh (2022), Varki, Ajit; Cummings, Richard D.; Esko, Jeffrey D.; Stanley, Pamela (eds.),"Glycosphingolipids",Essentials of Glycobiology (4th ed.), Cold Spring Harbor (NY): Cold Spring Harbor Laboratory Press,ISBN 978-1-62182-421-3,PMID 35536927, retrieved2024-09-10
  3. ^Harayama, Takeshi; Riezman, Howard (May 2018)."Understanding the diversity of membrane lipid composition".Nature Reviews. Molecular Cell Biology.19 (5):281–296.doi:10.1038/nrm.2017.138.ISSN 1471-0080.PMID 29410529.
  4. ^|SIGMA&N5=SEARCH_CONCAT_PNO|BRAND_KEY&F=SPEC Product page at Sigma Aldrich
  5. ^Dickson RC (1998)."Sphingolipid functions in Saccharomyces cerevisiae: comparison to mammals".Annual Review of Biochemistry.67:27–48.doi:10.1146/annurev.biochem.67.1.27.PMID 9759481.
  6. ^A brief, very comprehensible review is given in Gunstone, F. (1996)Fatty Acid and Lipid Chemistry, pp 43-44. Blackie Academic and Professional.ISBN 0-7514-0253-2
  7. ^Dickson RC (May 2008)."Thematic review series: sphingolipids. New insights into sphingolipid metabolism and function in budding yeast".Journal of Lipid Research.49 (5):909–21.doi:10.1194/jlr.R800003-JLR200.PMC 2311445.PMID 18296751.
  8. ^Bartke N, Hannun YA (April 2009)."Bioactive sphingolipids: metabolism and function".Journal of Lipid Research. 50 Suppl (Suppl): S91-6.doi:10.1194/jlr.R800080-JLR200.PMC 2674734.PMID 19017611.
  9. ^Merrill AH (December 1983). "Characterization of serine palmitoyltransferase activity in Chinese hamster ovary cells".Biochimica et Biophysica Acta (BBA) - Lipids and Lipid Metabolism.754 (3):284–91.doi:10.1016/0005-2760(83)90144-3.PMID 6652105.
  10. ^Merrill AH, Williams RD (February 1984)."Utilization of different fatty acyl-CoA thioesters by serine palmitoyltransferase from rat brain".Journal of Lipid Research.25 (2):185–8.doi:10.1016/S0022-2275(20)37838-X.PMID 6707526.
  11. ^Zitomer NC, Mitchell T, Voss KA, Bondy GS, Pruett ST, Garnier-Amblard EC, Liebeskind LS, Park H, Wang E, Sullards MC, Merrill AH, Riley RT (February 2009)."Ceramide synthase inhibition by fumonisin B1 causes accumulation of 1-deoxysphinganine: a novel category of bioactive 1-deoxysphingoid bases and 1-deoxydihydroceramides biosynthesized by mammalian cell lines and animals".The Journal of Biological Chemistry.284 (8):4786–95.doi:10.1074/jbc.M808798200.PMC 2643501.PMID 19095642.
  12. ^Pruett ST, Bushnev A, Hagedorn K, Adiga M, Haynes CA, Sullards MC, Liotta DC, Merrill AH (August 2008)."Biodiversity of sphingoid bases ("sphingosines") and related amino alcohols".Journal of Lipid Research.49 (8):1621–39.doi:10.1194/jlr.R800012-JLR200.PMC 2444003.PMID 18499644.
  13. ^Pewzner-Jung Y, Ben-Dor S, Futerman AH (September 2006)."When do Lasses (longevity assurance genes) become CerS (ceramide synthases)?: Insights into the regulation of ceramide synthesis".The Journal of Biological Chemistry.281 (35):25001–5.doi:10.1074/jbc.R600010200.PMID 16793762.
  14. ^Causeret C, Geeraert L, Van der Hoeven G, Mannaerts GP, Van Veldhoven PP (October 2000). "Further characterization of rat dihydroceramide desaturase: tissue distribution, subcellular localization, and substrate specificity".Lipids.35 (10):1117–25.doi:10.1007/s11745-000-0627-6.PMID 11104018.S2CID 3962533.
  15. ^Hannun YA, Obeid LM (February 2008). "Principles of bioactive lipid signalling: lessons from sphingolipids".Nature Reviews Molecular Cell Biology.9 (2):139–50.doi:10.1038/nrm2329.PMID 18216770.S2CID 8692993.
  16. ^Bandhuvula P, Saba JD (May 2007). "Sphingosine-1-phosphate lyase in immunity and cancer: silencing the siren".Trends in Molecular Medicine.13 (5):210–7.doi:10.1016/j.molmed.2007.03.005.PMID 17416206.
  17. ^Hannun YA, Obeid LM (July 2002)."The Ceramide-centric universe of lipid-mediated cell regulation: stress encounters of the lipid kind".The Journal of Biological Chemistry.277 (29):25847–50.doi:10.1074/jbc.R200008200.PMID 12011103.
  18. ^Spiegel S, Milstien S (July 2002)."Sphingosine 1-phosphate, a key cell signaling molecule".The Journal of Biological Chemistry.277 (29):25851–4.doi:10.1074/jbc.R200007200.PMID 12011102.
  19. ^Lavieu G, Scarlatti F, Sala G, Carpentier S, Levade T, Ghidoni R, Botti J, Codogno P (March 2006)."Regulation of autophagy by sphingosine kinase 1 and its role in cell survival during nutrient starvation".The Journal of Biological Chemistry.281 (13):8518–27.doi:10.1074/jbc.M506182200.PMID 16415355.
  20. ^Venable ME, Lee JY, Smyth MJ, Bielawska A, Obeid LM (December 1995)."Role of ceramide in cellular senescence".The Journal of Biological Chemistry.270 (51):30701–8.doi:10.1074/jbc.270.51.30701.PMID 8530509.
  21. ^Snider AJ, Orr Gandy KA, Obeid LM (June 2010)."Sphingosine kinase: Role in regulation of bioactive sphingolipid mediators in inflammation".Biochimie.92 (6):707–15.doi:10.1016/j.biochi.2010.02.008.PMC 2878898.PMID 20156522.
  22. ^Brown DA, London E (June 2000)."Structure and function of sphingolipid- and cholesterol-rich membrane rafts".The Journal of Biological Chemistry.275 (23):17221–4.doi:10.1074/jbc.R000005200.PMID 10770957.
  23. ^Futerman AH (December 2006)."Intracellular trafficking of sphingolipids: relationship to biosynthesis".Biochimica et Biophysica Acta (BBA) - Biomembranes.1758 (12):1885–92.doi:10.1016/j.bbamem.2006.08.004.PMID 16996025.
  24. ^van Meer G, Lisman Q (July 2002)."Sphingolipid transport: rafts and translocators".The Journal of Biological Chemistry.277 (29):25855–8.doi:10.1074/jbc.R200010200.PMID 12011105.
  25. ^Vesper H, Schmelz EM, Nikolova-Karakashian MN, Dillehay DL, Lynch DV, Merrill AH (July 1999)."Sphingolipids in food and the emerging importance of sphingolipids to nutrition".The Journal of Nutrition.129 (7):1239–50.doi:10.1093/jn/129.7.1239.PMID 10395583.
  26. ^Heaver, SL; Johnson, EL; Ley, RE (June 2018)."Sphingolipids in host-microbial interactions"(PDF).Current Opinion in Microbiology.43:92–99.doi:10.1016/j.mib.2017.12.011.PMID 29328957.S2CID 26181993.
  27. ^Chung N, Mao C, Heitman J, Hannun YA, Obeid LM (September 2001)."Phytosphingosine as a specific inhibitor of growth and nutrient import in Saccharomyces cerevisiae".The Journal of Biological Chemistry.276 (38):35614–21.doi:10.1074/jbc.m105653200.PMID 11468289.
  28. ^Cowart LA, Obeid LM (March 2007)."Yeast sphingolipids: recent developments in understanding biosynthesis, regulation, and function".Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids.1771 (3):421–31.doi:10.1016/j.bbalip.2006.08.005.PMC 1868558.PMID 16997623.
  29. ^Dickson RC (May 2008)."Thematic review series: sphingolipids. New insights into sphingolipid metabolism and function in budding yeast".Journal of Lipid Research.49 (5):909–21.doi:10.1194/jlr.R800003-JLR200.PMC 2311445.PMID 18296751.
  30. ^Brice SE, Alford CW, Cowart LA (March 2009)."Modulation of sphingolipid metabolism by the phosphatidylinositol-4-phosphate phosphatase Sac1p through regulation of phosphatidylinositol in Saccharomyces cerevisiae".The Journal of Biological Chemistry.284 (12):7588–96.doi:10.1074/jbc.M808325200.PMC 2658053.PMID 19139096.
  31. ^Chen K, Ho TS, Lin G, Tan KL, Rasband MN, Bellen HJ (November 2016)."Loss of Frataxin activates the iron/sphingolipid/PDK1/Mef2 pathway in mammals".eLife.5.doi:10.7554/eLife.20732.PMC 5130293.PMID 27901468.
  32. ^Chen K, Lin G, Haelterman NA, Ho TS, Li T, Li Z, Duraine L, Graham BH, Jaiswal M, Yamamoto S, Rasband MN, Bellen HJ (June 2016)."Loss of Frataxin induces iron toxicity, sphingolipid synthesis, and Pdk1/Mef2 activation, leading to neurodegeneration".eLife.5.doi:10.7554/eLife.16043.PMC 4956409.PMID 27343351.
  33. ^Esfandiary, Ali; Finkelstein, David Isaac; Voelcker, Nicolas Hans; Rudd, David (2022-04-15)."Clinical Sphingolipids Pathway in Parkinson's Disease: From GCase to Integrated-Biomarker Discovery".Cells.11 (8): 1353.doi:10.3390/cells11081353.ISSN 2073-4409.PMC 9028315.PMID 35456032.

External links

edit
[8]ページ先頭
©2009-2025 Movatter.jp