Comparative genomic hybridization of ductal carcinomain situ of the breast?evidence of multiple genetic pathways

Horst Buerger(University of Münster), Friedrich Otterbach(Institut Kurz), Ronald Simon(Institut Kurz), Christopher Poremba(Institut Kurz), Raihanatou Diallo(University of Münster), Thomas Decker(Helios Hospital Berlin-Buch), Lutz Riethdorf(Universität Hamburg), C. Brinkschmidt(Institut Kurz), Barbara Dockhorn‐Dworniczak(Institut Kurz), Werner Boecker(Institut Kurz)
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Abstract

There is strong evidence that ductal carcinoma in situ (DCIS) represents a precursor lesion of invasive breast cancer. In order to analyse specific chromosomal alterations of DCIS, 38 paraffin-embedded specimens of DCIS and six associated invasive carcinomas were examined by means of comparative genomic hybridization (CGH). Losses of 16q material were seen almost exclusively in well- and intermediately-differentiated DCIS. These two subgroups differed in the average number of genetic imbalances, 2.5 and 5.5 respectively. Additionally, a higher frequency of gains of 1q and losses of 11q material was seen in intermediately-differentiated in contrast to well-differentiated DCIS. Poorly-differentiated DCIS displayed a higher frequency of amplifications (17q12, 11q13) and a higher average rate of genetic imbalances (7.1). Analysis of adjacent invasive breast carcinoma revealed a genetic pattern almost identical to the one seen in the DCIS counterpart. These data characterize DCIS as a genetically far-advanced, heterogeneous lesion and as a direct precursor of invasive breast cancer.


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