Title of article
Molecular cytogenetic analysis of breast cancer: a combined multicolor fluorescence in situ hybridization and G-banding study of uncultured tumor cells
Author/Authors
Ferti، نويسنده , , Angeliki D. and Stamouli، نويسنده , , Maria J. and Panani، نويسنده , , Anna D. and Raptis، نويسنده , , Sotirios A. and Young، نويسنده , , Bryan D.، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2004
Pages
10
From page
28
To page
37
Abstract
In six patients with breast cancer, uncultured tumor cells were investigated with G-banding and multicolor fluorescence in situ hybridization (M-FISH). A large number of numerical and structural aberrations could be analyzed. Among other structural abnormalities, reciprocal, hidden and complex translocations were found. Recurrent t(1;10) and t(6;16), not previously described, were identified, as well as t(15;22). The latter was also found in additional cases among our unpublished breast carcinomas. The significance of t(15;22) for breast cancer is discussed, taking into account also data drawn from the literature. Reciprocal translocations were a prominent feature in a pseudodiploid lobular carcinoma. Hidden translocations on 6p22∼p24 were detected with M-FISH. Involvement of 6p22∼p24 was observed in five cases. The analysis of various other translocations and different structural abnormalities revealed the following common breakpoints (according to frequency of involvement): 1p34∼p36, 3p12∼p13, 4p13→q11, 14p11→q11, 1q42, 8p11, 8q24, 10q22, 11q13, 11q23∼q24, 13q13, and 18p10∼p11. Loss of 3p and 1p34∼p36→pter and complete or partial loss of 13q and chromosome 17 were also found. With the combination of G-banding and M-FISH techniques, chromosome misclassification is avoided and the characterization of complex tumor karyotypes is more effective.
Journal title
Cancer Genetics and Cytogenetics
Serial Year
2004
Journal title
Cancer Genetics and Cytogenetics
Record number
1825786
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