Una Gilvarry scite author profile

Una Gilvarry

3Publications

43Citation Statements Received

11Citation Statements Given

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Dublin City University

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Multiple drug-resistance in variant of a human non-small cell lung carcinoma cell line, DLKP-A

et al. 1992

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A 300-fold adriamycin resistant variant (DLKP-A) of the human lung squamous cell carcinoma line DLKP was established by stepwise selection in increasing concentrations of adriamycin. Different levels of cross-resistance were observed towards VP-16, VM-26, colchicine, vincristine and, somewhat unexpectedly, cis-platin. Resistance was stable for at least 3 months in culture in the absence of drug. P-glycoprotein overexpression was detected by immunofluorescence and Western Blotting, and a direct causal role for P-glycoprotein overexpression in the resistant phenotype was established by transfection with an mdr1 specific antisense oligonucleotide. A modified cryopreservation procedure was necessary for the resistant variant line. The resistant population displays clonal heterogeneity with respect to resistance level. A higher frequency of double minute chromosomes was observed in DLKP-A when compared with the parental cell line.

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Cytogenetic comparison of two poorly differentiated human lung squamous cell carcinoma lines

Law

Gilvarry

Lynch

et al. 1992

Cancer Genetics and Cytogenetics

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Establishment of two new multi-drug resistant variants of the human tumor line Hep-2

et al. 1990

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Two multi-drug resistant variants of the human carcinoma line Hep-2 have been selected by adaptation to progressively increasing concentrations of adriamycin. In comparison to the wild-type Hep-2 cells, the variant lines both showed approximately 100-fold resistance to adriamycin, 10 to 20-fold resistance to the vinca alkaloids but only 2-3 fold resistance to VP-16 and VM-26. There was essentially no difference between wild-type and variant cells in regard to sensitivity to threosulfan and 5-fluorouracil. The drug-resistant phenotype is stable for at least 3 months in the absence of drug, and is partially reversible by concomitant treatment with Verapamil. Chromosomal abnormalities consistent with gene amplification were observed in one of the variant lines. Sensitivity of variant cells to adriamycin was enhanced following trypsin-EDTA treatment.

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Una Gilvarry

Multiple drug-resistance in variant of a human non-small cell lung carcinoma cell line, DLKP-A

Cytogenetic comparison of two poorly differentiated human lung squamous cell carcinoma lines

Establishment of two new multi-drug resistant variants of the human tumor line Hep-2

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