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Tumor spreading to the contralateral ovary in bilateral ovarian carcinoma is a late event in clonal evolution.
Micci, Francesca; Haugom, Lisbeth; Ahlquist, Terje; Abeler, Vera M; Trope, Claes G; Lothe, Ragnhild A; Heim, Sverre.
  • Micci F; Department of Medical Genetics, The Norwegian Radium Hospital, Oslo University Hospital, 0310 Oslo, Norway.
J Oncol ; 2010: 646340, 2010.
Article en En | MEDLINE | ID: mdl-19759843
ABSTRACT
Cancer of the ovary is bilateral in 25%. Cytogenetic analysis could determine whether the disease in bilateral cases is metastatic or two separately occurring primary tumors, but karyotypic information comparing the two cancerous ovaries is limited to a single report with 11 informative cases. We present a series of 32 bilateral ovarian carcinoma cases, analyzed by karyotyping and high-resolution CGH. Our karyotypic findings showed that spreading to the contralateral ovary had occurred in bilateral ovarian cancer cases and that it was a late event in the clonal evolution of the tumors. This was confirmed by the large number of similar changes detected by HR-CGH in the different lesions from the same patient. The chromosomal bands most frequently involved in structural rearrangements were 19p13 (n = 12) and 19q13 (n = 11). The chromosomal bands most frequently gained by both tumorous ovaries were 5p14 (70%), 8q23-24 (65%), 1q23-24 (57%), and 12p12 (48%), whereas the most frequently lost bands were 17p11 (78%), 17p13 (74%), 17p12 (70%), 22q13 (61%), 8p21 and 19q13 (52%), and 8p22-23 (48%). This is the first time that 5p14 is seen gained at such a high frequency in cancer of the ovary; possibly oncogene(s) involved in bilateral ovarian carcinogenesis or tumor progression may reside in this band.