Variation in topoisomerase I gene copy number as a mechanism for intrinsic drug sensitivity | Zendy

H. L. McLeod | Zendy; W. Nicol Keith | Zendy

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Variation in topoisomerase I gene copy number as a mechanism for intrinsic drug sensitivity

Author(s) -

H. L. McLeod,

W. Nicol Keith

Publication year - 1996

Publication title -

british journal of cancer

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.833

H-Index - 236

eISSN - 1532-1827

pISSN - 0007-0920

DOI - 10.1038/bjc.1996.394

Subject(s) - polysomy , copy number variation , biology , topoisomerase , camptothecin , gene , gene duplication , gene dosage , genetics , locus (genetics) , dna , isochromosome , drug resistance , gene expression , microbiology and biotechnology , chromosome , biochemistry , genome , in situ hybridization , karyotype

DNA topoisomerase I (topo I) is the principle target for camptothecin and its derivatives such as SN38. Levels of topo I expression vary widely between and within tumour types and the basis for this is poorly understood. We have used fluorescence in situ hybridisation to detect the topo I locus in a panel of breast and colon cancer cell lines. This approach has identified a range of topo I gene copies from 1 to 6 between the cell lines as a result of DNA amplification, polysomy and isochromosome formation. Topo I gene copy number was highly correlated with topo I expression, (rs = 0.92), and inversely correlated to sensitivity to a 1 h exposure to SN38 (rs = -0.904). This illustrates the significant impact of altered topo I gene copy number on intrinsic drug sensitivity and influences potential mechanisms for acquisition of drug resistance.

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