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    Pre-Invasive Ovarian Mucinous Tumors Are Characterized by CDKN2A and RAS Pathway Aberrations

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    Author
    Hunter, SM; Gorringe, KL; Christie, M; Rowley, SM; Bowtell, DD; Campbell, IG
    Date
    2012-10-01
    Source Title
    CLINICAL CANCER RESEARCH
    Publisher
    AMER ASSOC CANCER RESEARCH
    University of Melbourne Author/s
    Campbell, Ian; Christie, Michael; Gorringe, Kylie; Bowtell, David
    Affiliation
    Biochemistry and Molecular Biology
    Pathology
    Metadata
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    Document Type
    Journal Article
    Citations
    Hunter, SM; Gorringe, KL; Christie, M; Rowley, SM; Bowtell, DD; Campbell, IG, Pre-Invasive Ovarian Mucinous Tumors Are Characterized by CDKN2A and RAS Pathway Aberrations, CLINICAL CANCER RESEARCH, 2012, 18 (19), pp. 5267 - 5277
    Access Status
    Open Access
    URI
    http://hdl.handle.net/11343/43906
    DOI
    10.1158/1078-0432.CCR-12-1103
    NHMRC Grant code
    NHMRC/628630
    NHMRC/400413
    Abstract
    INTRODUCTION: Mucinous tumors are the second most common form of epithelial ovarian tumor, yet the cell of origin for this histologic subtype remains undetermined. Although these tumors are thought to arise through a stepwise progression from benign cystadenoma to borderline tumor to invasive carcinoma, few studies have attempted to comprehensively characterize the genetic changes specific to this subtype or its precursors. METHODS: To explore the spectrum of genomic alterations common to mucinous tumors we carried out high-resolution genome-wide copy number analysis, mutation screening by Sanger sequencing and immunohistochemistry on a series of primary ovarian mucinous cystadenomas (n = 20) and borderline tumors (n = 22). RESULTS: Integration of copy number data, targeted mutation screening of RAS/RAF pathway members and immunohistochemistry reveals that p16 loss and RAS/RAF pathway alterations are highly recurrent events that occur early during mucinous tumor development. The frequency of concurrence of these events was observed in 40% of benign cystadenomas and 68% of borderline tumors. CONCLUSIONS: This study is the largest and highest resolution analysis of mucinous benign and borderline tumors carried out to date and provides strong support for these lesions being precursors of primary ovarian mucinous adenocarcinoma. The high level of uniformity in the molecular events underlying the pathogenesis of mucinous ovarian tumors provides an opportunity for treatments targeting specific mutations and pathways.

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