Literature DB >> 15514480

Integration of glycosphingolipid metabolism and cell-fate decisions in cancer and stem cells: review and hypothesis.

Erhard Bieberich1.   

Abstract

The metabolism of glycosphingolipids is strictly regulated during the mitotic cell cycle. Before the G1-to-S transition, the ceramide and glucosylceramide concentration is elevated. Ceramide induces apoptosis synergistically with the pro-apoptotic protein prostate apoptosis response 4 (PAR-4) that may be asymmetrically inherited during cell division. Only one daughter cell dies shortly after mitosis, a mechanism we suggested to regulate the number of neural stem cells during embryonic development. The progeny cells, however, may protect themselves by converting ceramide to glucosylceramide and other glycosphingolipids. In particular, complex gangliosides have been found to sustain cell survival and differentiation. The cell cycle may thus be a turning point for (glyco)sphingolipid metabolism and explain rapid changes of the sphingolipid composition in cells that undergo mitotic cell-fate decisions. In the proposed model termed "Shiva cycle", progression through the cell cycle, differentiation, or apoptosis may rely on a delicate balance of (glyco)sphingolipid second messengers that modulate the retinoblastoma-dependent G1-to-S transition or caspase-dependent G1-to-apoptosis program. Ceramide-induced cell cycle delay at G0/G1 is either followed by ceramide-induced apoptosis or by conversion of ceramide to glucosylceramide, a proposed key regulatory rheostat that rescues cells from re-entry into a life/death decision at G1-to-S. We propose a mechanistic model for sphingolpid-induced protein scaffolds ("slip") that regulate cell-fate decisions and will discuss the biological consequences and pharmacological potential of manipulating the (glyco)sphingolipid-dependent cell fate program in cancer and stem cells.

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Year:  2004        PMID: 15514480     DOI: 10.1023/B:GLYC.0000046274.35732.47

Source DB:  PubMed          Journal:  Glycoconj J        ISSN: 0282-0080            Impact factor:   2.916


  142 in total

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3.  Molecular mechanisms of ceramide-mediated telomerase inhibition in the A549 human lung adenocarcinoma cell line.

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4.  Synthesis and characterization of novel ceramide analogs for induction of apoptosis in human cancer cells.

Authors:  Erhard Bieberich; Bin Hu; Jeane Silva; Sarah MacKinnon; Robert K Yu; Helen Fillmore; William C Broaddus; Raphael M Ottenbrite
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5.  Sphingolipid depletion increases formation of the scrapie prion protein in neuroblastoma cells infected with prions.

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6.  Intracerebroventricular administration of GM1 ganglioside to presenile Alzheimer patients.

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Review 8.  Tumor-associated carbohydrate antigens defining tumor malignancy: basis for development of anti-cancer vaccines.

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10.  Bax deletion further orders the cell death pathway in cerebellar granule cells and suggests a caspase-independent pathway to cell death.

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  25 in total

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2.  Elastase 2 is expressed in human and mouse epidermis and impairs skin barrier function in Netherton syndrome through filaggrin and lipid misprocessing.

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Review 3.  Sphingolipids and expression regulation of genes in cancer.

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4.  Sialidase NEU3 is a peripheral membrane protein localized on the cell surface and in endosomal structures.

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Review 6.  Ceramide glycosylation catalyzed by glucosylceramide synthase and cancer drug resistance.

Authors:  Yong-Yu Liu; Ronald A Hill; Yu-Teh Li
Journal:  Adv Cancer Res       Date:  2013       Impact factor: 6.242

Review 7.  Sphingolipids and lipid rafts: Novel concepts and methods of analysis.

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Review 8.  It's a lipid's world: bioactive lipid metabolism and signaling in neural stem cell differentiation.

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9.  Ceramide signaling in cancer and stem cells.

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10.  Transcript profiling and lipidomic analysis of ceramide subspecies in mouse embryonic stem cells and embryoid bodies.

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