Inhibition of Multidrug Resistance by AdamantylGb3, a Globotriaosylceramide Analog

Rosa, María Fabiana De; Ackerley, Cameron; Wang, Bernice; Itô, Shinya; Clarke, David M.; Lingwood, Clifford A.

doi:10.1074/jbc.m705473200

Cited by 38 publications

(41 citation statements)

References 75 publications

(93 reference statements)

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“…We could also correlate increased expression of Gb3 of cisplatin-resistant MPM and NSCLC cells to increased expression of MDR1/PgP. Gb3 and MDR1/PgP have recently been found to be partially co-localised in MDR1/PgPexpressing cells, and Gb3-containing lipid rafts are important for intracellular MDR1/PgP surface trafficking (De Rosa et al, 2008). The increased expression of MDR1/PgP in cisplatin resistance could, therefore, parallel increased Gb3 expression, as MDR1/PgP acts as a glycolipid translocase involved in the biosynthesis of glycolipids such as Gb3 (De Rosa et al, 2008).…”

Section: Discussionmentioning

confidence: 70%

“…Gb3 and MDR1/PgP have recently been found to be partially co-localised in MDR1/PgPexpressing cells, and Gb3-containing lipid rafts are important for intracellular MDR1/PgP surface trafficking (De Rosa et al, 2008). The increased expression of MDR1/PgP in cisplatin resistance could, therefore, parallel increased Gb3 expression, as MDR1/PgP acts as a glycolipid translocase involved in the biosynthesis of glycolipids such as Gb3 (De Rosa et al, 2008). However, we found also particularly of the Gb3-expressing fraction that was induced when the mother cell line was made cisplatin resistant.…”

Section: Discussionmentioning

confidence: 99%

“…MDR1/PgP acts as a glycolipid translocase involved in the biosynthesis of glycolipids such as Gb3, and elevated levels of Gb3 have also been seen in drug-resistant cancers, and functional interplay between membrane Gb3 and MDR1/PgP has been suggested (Lingwood et al, 1998;De Rosa et al, 2008). Gb3 functions as cell surface receptor for verotoxin-1 (VT-1, Shiga-like toxin-1) produced by pathogenic strains of Escherichia coli (Lingwood et al, 1987;Jacewicz et al, 1989;Rose and Clark, 1989).…”

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Cisplatin-induced expression of Gb3 enables verotoxin-1 treatment of cisplatin resistance in malignant pleural mesothelioma cells

et al. 2009

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BACKGROUND: A major problem with cisplatin treatment is the development of acquired-drug resistance of the tumour cells. Verotoxin-1 (VT-1) exerts its cytotoxicity by targeting the membrane glycolipid globotriasosylceramide (Gb3), a molecule associated with drug resistance. Cisplatin-and VT-1-induced apoptosis involves mitogen-activated protein kinase (MAPK) activation, and deactivation of MAPKs is associated with cisplatin resistance. This study aimed to investigate whether a sub-toxic concentration of VT-1 could enhance cisplatin-induced apoptosis and overcome acquired-cisplatin resistance in cultured cancer cell lines. METHOD: P31 and H1299 cells with corresponding cisplatin-resistant sub-lines (P31res/H1299res) were incubated with VT-1 and/or cisplatin followed by determination of Gb3 expression, cell viability, apoptosis, and signalling pathways. RESULTS: Cells from the resistant sub-lines had elevated Gb3 expression compared with the parental cell lines, and cisplatin further increased Gb3 expression, whereas VT-1 reduced the percentage of Gb3-expressing cells. Combination of cisplatin and sub-toxic concentrations of VT-1 led to a super-additive increase of cytotoxicity and TUNEL staining, especially in the cisplatin-resistant sublines. Blockade of Gb3 synthesis by a Gb3 synthesis inhibitor not only led to eradicated TUNEL staining of P31 cells, but also sensitised P31res cells to the induction of apoptosis by cisplatin alone. Cisplatin-and VT-1-induced apoptosis involved the MAPK pathways with increased C-Jun N-terminal kinase and MAPK kinase-3 and -6 phosphorylation. CONCLUSIONS: We show the presence of Gb3 in acquired-cisplatin resistance in P31res and H1299res cells. Cisplatin up-regulated Gb3 expression in all cells and thus sensitised the cells to VT-1-induced cytotoxicity. A strong super-additive effect of combined cisplatin and a sub-toxic concentration of VT-1 in cisplatin-resistant malignant pleural mesothelioma cells were observed, indicating a new potential clinical-treatment approach.

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Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Cisplatin-induced expression of Gb3 enables verotoxin-1 treatment of cisplatin resistance in malignant pleural mesothelioma cells

et al. 2009

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“…efflux, indicating that the lipid-binding site interferes with substrate binding (De Rosa et al, 2008). ABCB1 partially colocalizes with globotriaosylceramide at the cell surface, and glycosphingolipid depletion results in a decreased cell surface expression of ABCB1, indicating that gangliosides also influence the trafficking of this protein.…”

Section: Article In Pressmentioning

confidence: 99%

Lipid Regulation of the ABCB1 and ABCG2 Multidrug Transporters

Hegedüs

Telbisz

Hegedüs

et al. 2015

Advances in Cancer Research

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“…In SGC7901/AS, only ABCB1 appeared to have significant expression at both the transcriptional and the translational level. Although there was no significant inhibition of growth in two arsenic-resistant cell lines with 20 μM verapamil, a standard ABCB1 inhibitor (26), two resistant cell lines partially restored the sensitivity of As 2 O 3 under 50 μM verapamil. The survival in the resistant group was still 10 to 20% higher than that in wild-type group.…”

Section: Discussionmentioning

confidence: 99%

The overexpression of multidrug resistance-associated proteins and gankyrin contribute to arsenic trioxide resistance in liver and gastric cancer cells

Chen

Zhang²,

Liu³

2009

Oncol Rep

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Abstract. Arsenic trioxide has been used as a therapeutic agent for acute promyelocytic leukemia and recently for some solid tumors. Although arsenic trioxide has been shown to significantly inhibit the growth of solid tumor cells in vitro, clinical trials indicate that arsenic trioxide alone is pool active against non-hematologic malignant diseases. To understand the mechanisms of arsenic resistance in solid tumor cells, we established two arsenic-resistant solid tumor cell lines, HepG2/AS and SGC7901/AS, isolated from human liver cancer cell line HepG2 and human gastric cancer cell line SGC7901, respectively, by a series of stepwise selections via treatment with increasing concentrations of arsenic trioxide. Three ABC transporter proteins, ABCB1, ABCC1 and ABCC2, were expressed increasingly and differently in two arsenic-resistant cell lines. Further, tumor suppressor p53 was overexpressed in two arsenic-resistant cell lines, but the levels of p53 mediators MDM2 and gankyrin, which regulate the ubiquitination of p53, increased simultaneously. In addition, an increase in the phosphorylation of Rb at Ser795 in the two cell lines might also result from the presence of MDM2 and gankyrin, which suggest that the inactivation of p53 and Rb contribute to drug resistance. These two arsenic-resistant solid tumor cell lines, HepG2/AS and SGC7901/AS, may be useful for studying the mechanism of arsenic resistance in solid tumors and may provide a way to overcome it.

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Inhibition of Multidrug Resistance by AdamantylGb3, a Globotriaosylceramide Analog

Cited by 38 publications

References 75 publications

Cisplatin-induced expression of Gb3 enables verotoxin-1 treatment of cisplatin resistance in malignant pleural mesothelioma cells

Cisplatin-induced expression of Gb3 enables verotoxin-1 treatment of cisplatin resistance in malignant pleural mesothelioma cells

Lipid Regulation of the ABCB1 and ABCG2 Multidrug Transporters

The overexpression of multidrug resistance-associated proteins and gankyrin contribute to arsenic trioxide resistance in liver and gastric cancer cells

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