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Literature DB >> 12374201

Sphingolipids in neuroblastoma: their role in drug resistance mechanisms.

Hannie Sietsma¹, Anne Jan Dijkhuis, Willem Kamps, Jan Willem Kok.

Abstract

Disseminated neuroblastoma usually calls for chemotherapy as the primary approach for treatment. Treatment failure is often attributable to drug resistance. This involves a variety of cellular mechanisms, including increased drug efflux through expression of ATP-binding cassette transporters (e.g., P-glycoprotein) and the inability of tumor cells to activate or propagate the apoptotic response. In recent years it has become apparent that sphingolipid metabolism and the generation of sphingolipid species, such as ceramide, also play a role in drug resistance. This may involve an autonomous mechanism, related to direct effects of sphingolipids on the apoptotic response, but also a subtle interplay between sphingolipids and ATP-binding cassette transporters. Here, we present an overview of the current understanding of the multiple levels at which sphingolipids function in drug resistance, with an emphasis on sphingolipid function in neuroblastoma and how modulation of sphingolipid metabolism may be used as a novel treatment paradigm.

Entities: Chemical Disease Gene

Mesh：

Substances：
Sphingolipids

Year: 2002 PMID： 12374201 DOI： 10.1023/a:1020228117739

Source DB: PubMed Journal: Neurochem Res ISSN： 0364-3190 Impact factor: 3.996

87 in total

Review 1. Analysis of the tangled relationships between P-glycoprotein-mediated multidrug resistance and the lipid phase of the cell membrane.

Authors: J Ferté
Journal: Eur J Biochem Date: 2000-01

2. Agents that reverse multidrug resistance, tamoxifen, verapamil, and cyclosporin A, block glycosphingolipid metabolism by inhibiting ceramide glycosylation in human cancer cells.

Authors: Y Lavie; H t Cao; A Volner; A Lucci; T Y Han; V Geffen; A E Giuliano; M C Cabot
Journal: J Biol Chem Date: 1997-01-17 Impact factor: 5.157

Review 3. Tumor malignancy defined by aberrant glycosylation and sphingo(glyco)lipid metabolism.

Authors: S Hakomori
Journal: Cancer Res Date: 1996-12-01 Impact factor: 12.701

4. MDR1 P-glycoprotein is a lipid translocase of broad specificity, while MDR3 P-glycoprotein specifically translocates phosphatidylcholine.

Authors: A van Helvoort; A J Smith; H Sprong; I Fritzsche; A H Schinkel; P Borst; G van Meer
Journal: Cell Date: 1996-11-01 Impact factor: 41.582

5. Neuroblastoma-derived gangliosides inhibit dendritic cell generation and function.

Authors: G V Shurin; M R Shurin; S Bykovskaia; J Shogan; M T Lotze; E M Barksdale
Journal: Cancer Res Date: 2001-01-01 Impact factor: 12.701

6. The p75(NTR)-induced apoptotic program develops through a ceramide-caspase pathway negatively regulated by nitric oxide.

Authors: J P Lièvremont; C Sciorati; E Morandi; C Paolucci; G Bunone; G Della Valle; J Meldolesi; E Clementi
Journal: J Biol Chem Date: 1999-05-28 Impact factor: 5.157

7. Altered expression of the MYCN oncogene modulates MRP gene expression and response to cytotoxic drugs in neuroblastoma cells.

Authors: M Haber; S B Bordow; J Gilbert; J Madafiglio; M Kavallaris; G M Marshall; E B Mechetner; J P Fruehauf; L Tee; S L Cohn; H Salwen; M L Schmidt; M D Norris
Journal: Oncogene Date: 1999-04-29 Impact factor: 9.867

8. Restoration of TNF-alpha-induced ceramide generation and apoptosis in resistant human leukemia KG1a cells by the P-glycoprotein blocker PSC833.

Authors: C Bezombes; N Maestre; G Laurent; T Levade; A Bettaïeb; J P Jaffrézou
Journal: FASEB J Date: 1998-01 Impact factor: 5.191

9. Inhibition of hemopoiesis in vitro by neuroblastoma-derived gangliosides.

Authors: H Sietsma; W Nijhof; B Dontje; E Vellenga; W A Kamps; J W Kok
Journal: Cancer Res Date: 1998-11-01 Impact factor: 12.701

10. The human MDR3 P-glycoprotein promotes translocation of phosphatidylcholine through the plasma membrane of fibroblasts from transgenic mice.

Authors: A J Smith; J L Timmermans-Hereijgers; B Roelofsen; K W Wirtz; W J van Blitterswijk; J J Smit; A H Schinkel; P Borst
Journal: FEBS Lett Date: 1994-11-14 Impact factor: 4.124

5 in total

Sphingolipids in neuroblastoma: their role in drug resistance mechanisms.

Review 1. Analysis of the tangled relationships between P-glycoprotein-mediated multidrug resistance and the lipid phase of the cell membrane.

2. Agents that reverse multidrug resistance, tamoxifen, verapamil, and cyclosporin A, block glycosphingolipid metabolism by inhibiting ceramide glycosylation in human cancer cells.

Review 3. Tumor malignancy defined by aberrant glycosylation and sphingo(glyco)lipid metabolism.

4. MDR1 P-glycoprotein is a lipid translocase of broad specificity, while MDR3 P-glycoprotein specifically translocates phosphatidylcholine.

5. Neuroblastoma-derived gangliosides inhibit dendritic cell generation and function.

6. The p75(NTR)-induced apoptotic program develops through a ceramide-caspase pathway negatively regulated by nitric oxide.

7. Altered expression of the MYCN oncogene modulates MRP gene expression and response to cytotoxic drugs in neuroblastoma cells.

8. Restoration of TNF-alpha-induced ceramide generation and apoptosis in resistant human leukemia KG1a cells by the P-glycoprotein blocker PSC833.

9. Inhibition of hemopoiesis in vitro by neuroblastoma-derived gangliosides.

10. The human MDR3 P-glycoprotein promotes translocation of phosphatidylcholine through the plasma membrane of fibroblasts from transgenic mice.

Review 1. Tamoxifen regulation of sphingolipid metabolism--Therapeutic implications.

2. Potential anti-neuroblastoma agents from Juniperus oblonga.

3. A new glucoceramide from the watermelon Begonia, Pellionia repens.

4. Ceramide and glucosylceramide upregulate expression of the multidrug resistance gene MDR1 in cancer cells.

Review 5. New approaches to pharmacotherapy of tumors of the nervous system during childhood and adolescence.