4.6 Article

Molecular classification of high grade endometrioid and clear cell ovarian cancer using TCGA gene expression signatures

Journal

GYNECOLOGIC ONCOLOGY
Volume 141, Issue 1, Pages 95-100

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ygyno.2016.02.023

Keywords

Ovarian cancer; Molecular subtypes; Endometrioid; Clear cell and high grade serous histologies

Funding

  1. Dr. Miriam and Sheldon G. Adelson Medical Research Foundation
  2. Thelma L. Culverson Endowed Cancer Research Fund
  3. Stranahan Foundation for Translational Cancer Research and Advanced Clinical Cancer Research
  4. Fred C. and Katherine B. Andersen Foundation
  5. US National Institute of Health [P50 163393, R01 CA122443]
  6. Mayo Clinic Ovarian Cancer SPORE [P50 CA136393]

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Background. It is unclear whether the transcriptional subtypes of high grade serous ovarian cancer (HGSOC) apply to high grade clear cell (HGCCOC) or high grade endometrioid ovarian cancer (HGEOC). We aim to delineate transcriptional profiles of HGCCOCs and HGEOCs. Methods. We used Agilent microarrays to determine gene expression profiles of 276 well annotated ovarian cancers (OCs) including 37 HGCCOCs and 66 HGEOCs. We excluded low grade OCs as these are known to be distinct molecular entities. We applied the prespecified TCGA and CLOVAR gene signatures using consensus non negative matrix factorization (NMF). Results. We confirm the presence of four TCGA transcriptional subtypes and their significant prognostic relevance (p < 0.001) across all three histological subtypes (HGSOC, HGCCOC and HGEOCs). However, we also demonstrate that 22/37 (59%) HGCCOCs and 30/67 (45%) HGEOCs form 2 additional separate clusters with distinct gene signatures. importantly, of the HGCCOC and HGEOCs that clustered separately 62% and 65% were early stage (FIGOI/II), respectively. These finding were confirmed using the reduced CLOVAR gene set for classification where most early stage HGCCOCs and HGEOCs formed a distinct cluster of their own. When restricting the analysis to the four TCGA signatures (ssGSEA or NMF with CLOVAR genes) most early stage HGCCOCs and HGEOC were assigned to the differentiated subtype. Conclusions. Using transcriptional profiling the current study suggests that HGCCOCs and HGEOCs of advanced stage group together with HGSOCs. However, HGCCOCs and HGEOCs of early disease stages may have distinct transcriptional signatures similar to those seen in their low grade counterparts. (C) 2016 Elsevier Inc. All rights reserved.

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