2005
DOI: 10.1038/sj.bjc.6602228
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Multicolour-banding fluorescence in situ hybridisation (mbanding-FISH) to identify recurrent chromosomal alterations in breast tumour cell lines

Abstract: Recurrent chromosome breakpoints in tumour cells may point to cancer genes, but not many have been molecularly characterised. We have used multicolour-banding fluorescence in situ hybridisation (mbanding-FISH) on breast tumour cell lines to identify regions of chromosome break created by inversions, duplications, insertions and translocations on chromosomes 1, 5, 8, 12 and 17. We delineate a total of 136 regions of break, some of them occurring with high frequency. We further describe two examples of dualcolou… Show more

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Cited by 7 publications
(11 citation statements)
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References 52 publications
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“…Regions were considered to be gained or lost when at least two consecutive BAC clones presented a log 2 ratio > 0. 25 classified by hierarchical clustering (Fig. 3A).…”
Section: Gene Expression Profiling Revealed Overexpression Of 8p11-12mentioning
confidence: 99%
See 3 more Smart Citations
“…Regions were considered to be gained or lost when at least two consecutive BAC clones presented a log 2 ratio > 0. 25 classified by hierarchical clustering (Fig. 3A).…”
Section: Gene Expression Profiling Revealed Overexpression Of 8p11-12mentioning
confidence: 99%
“…We used dual-color FISH analysis with probes covering the region between NRG1 (not included) and FGFR1 ( Fig. 2F; Supplementary Table S4) in a series of 12 cell lines (Set 1, Supplementary Table S1) selected based on either the existence of transition in their aCGH profile or 8p11-21 rearrangement detected previously by mbanding FISH (25).…”
Section: Chromosome Breaks Are Associated With 8p Amplificationmentioning
confidence: 99%
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“…Previous publications describing the use of MCB include: diagnosis of a balanced CCR found in a healthy female as part of infertility investigations [Kuechler et al, 2005], prenatal diagnosis of a balanced CCR in an ICSI pregnancy [Trimborn et al, 2005], characterization of a 15‐breakpoint CCR in a mentally retarded child [Houge et al, 2003] and a multiple translocation event in a patient with hexadactyly, facial dysmorphism, mental retardation, and behavior disorder [Seidel et al, 2003], confirmation of a complex karyotype in a child with multiple congenital abnormalities [Kline et al, 2004], and the identification of recurrent chromosomal alterations in breast tumor cell lines [Letessier et al, 2005]. In the case described here, the structure of the derivative chromosome 12, together with the nature and extent of the monosomy, could not have been ascertained without the use of MCB; we are only aware of one other publication [Weise et al, 2002], describing such delineation of chromosomal monosomy in a constitutional karyotype.…”
Section: Discussionmentioning
confidence: 99%