Literature DB >> 10398423

Analysis of ovarian borderline tumors using comparative genomic hybridization and fluorescence in situ hybridization.

N G Wolf1, F W Abdul-Karim, C Farver, E Schröck, S du Manoir, S Schwartz.   

Abstract

It is unclear whether ovarian borderline tumors (tumors of low malignant potential) are independent entities or whether they are part of a continuum of tumor progression that culminates in ovarian carcinoma. Little is known about genetic abnormalities in borderline tumors because of the difficulty of growing them in culture for chromosome studies, and because the low ratio of tumor to nontumor cells can interfere with molecular genetic examination. To circumvent these problems, we performed comparative genomic hybridization (CGH) on 10 serous borderline tumors from nine patients, using microdissection to enrich the samples for tumor DNA and reduce contamination from stromal and inflammatory cells. CGH analysis revealed that three of the tumors had detectable chromosomal imbalances, whereas seven were in a balanced state. In those tumors with imbalances, the number of abnormalities ranged from 3-6 per tumor. Additional studies by fluorescence in situ hybridization (FISH) on disaggregated nuclei confirmed the imbalances detected by CGH, revealed one tumor to be hypertriploid, and indicated that the remaining tumors were diploid and in a balanced state. All abnormalities observed in the aneuploid cases are consistent with chromosomal aberrations previously reported for ovarian carinomas, providing further evidence that some borderline tumors are part of a continuum of tumor progression. These results also suggest that there may be different mechanisms leading to borderline tumor formation, including one associated with multiple chromosomal imbalances, and others that do not involve imbalances detectable by CGH. Genes Chromosomes Cancer 25:307-315, 1999. Copyright 1999 Wiley-Liss, Inc.

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Year:  1999        PMID: 10398423

Source DB:  PubMed          Journal:  Genes Chromosomes Cancer        ISSN: 1045-2257            Impact factor:   5.006


  7 in total

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2.  Genomic aberrations in borderline ovarian tumors.

Authors:  Francesca Micci; Lisbeth Haugom; Terje Ahlquist; Hege K Andersen; Vera M Abeler; Ben Davidson; Claes G Trope; Ragnhild A Lothe; Sverre Heim
Journal:  J Transl Med       Date:  2010-02-26       Impact factor: 5.531

3.  Gross genomic alterations differ between serous borderline tumors and serous adenocarcinomas--an image cytometric DNA ploidy analysis of 307 cases with histogenetic implications.

Authors:  Manohar Pradhan; Ben Davidson; Claes Göran Tropé; Håvard Emil Danielsen; Vera Maria Abeler; Björn Risberg
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4.  High Grade Serous Cystadenocarcinoma of Testis-Case Report of a Rare Ovarian Epithelial Type Tumour.

Authors:  Sithara Aravind; Sangeetha K Nayanar; R Varadharajaperumal; T V Satheeshbabu; Satheesan Balasubramanian
Journal:  J Clin Diagn Res       Date:  2017-06-01

5.  Chromosome 3 anomalies investigated by genome wide SNP analysis of benign, low malignant potential and low grade ovarian serous tumours.

Authors:  Ashley H Birch; Suzanna L Arcand; Kathleen K Oros; Kurosh Rahimi; A Kevin Watters; Diane Provencher; Celia M Greenwood; Anne-Marie Mes-Masson; Patricia N Tonin
Journal:  PLoS One       Date:  2011-12-06       Impact factor: 3.240

6.  Ovarian-type epithelial tumours of the testis: immunohistochemical and molecular analysis of two serous borderline tumours of the testis.

Authors:  Tobias Bürger; Hans-Ulrich Schildhaus; Reinhard Inniger; Joachim Hansen; Peter Mayer; Stefan Schweyer; Heinz Joachim Radzun; Philipp Ströbel; Felix Bremmer
Journal:  Diagn Pathol       Date:  2015-07-22       Impact factor: 2.644

7.  Genome profiling of ovarian adenocarcinomas using pangenomic BACs microarray comparative genomic hybridization.

Authors:  Donatella Caserta; Moncef Benkhalifa; Marina Baldi; Francesco Fiorentino; Mazin Qumsiyeh; Massimo Moscarini
Journal:  Mol Cytogenet       Date:  2008-05-20       Impact factor: 2.009

  7 in total

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