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Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome

In this study we aimed to analyze the biological mechanisms underlying apparently different modes of peritoneal tumor spread in serous ovarian cancer: miliary (widespread, millet-like lesions) versus non-miliary (bigger, exophytically growing implants). Tumor tissues and ascites from 23 chemotherapy...

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Autores principales: Auer, Katharina, Bachmayr-Heyda, Anna, Aust, Stefanie, Sukhbaatar, Nyamdelger, Reiner, Agnes Teresa, Grimm, Christoph, Horvat, Reinhard, Zeillinger, Robert, Pils, Dietmar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4627306/
https://www.ncbi.nlm.nih.gov/pubmed/25991672
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author Auer, Katharina
Bachmayr-Heyda, Anna
Aust, Stefanie
Sukhbaatar, Nyamdelger
Reiner, Agnes Teresa
Grimm, Christoph
Horvat, Reinhard
Zeillinger, Robert
Pils, Dietmar
author_facet Auer, Katharina
Bachmayr-Heyda, Anna
Aust, Stefanie
Sukhbaatar, Nyamdelger
Reiner, Agnes Teresa
Grimm, Christoph
Horvat, Reinhard
Zeillinger, Robert
Pils, Dietmar
author_sort Auer, Katharina
collection PubMed
description In this study we aimed to analyze the biological mechanisms underlying apparently different modes of peritoneal tumor spread in serous ovarian cancer: miliary (widespread, millet-like lesions) versus non-miliary (bigger, exophytically growing implants). Tumor tissues and ascites from 23 chemotherapy naive patients were analyzed by RNA-sequencing and flow cytometry. On the basis of differential gene expression between miliary and non-miliary, gene signatures were developed. A calculated tumor spread factor revealed a significant independent negative impact of miliary spread on overall survival (HR 3.77; CI(95) 1.14–12.39; p = 0.029) in an independent cohort of 165 serous ovarian cancer patients. Comparing previously published epithelial-mesenchymal transition (EMT) gene signatures, non-miliary spread correlated significantly with a reduced epithelial status. We conclude that serous ovarian cancer is a heterogeneous disease with distinct modes of peritoneal tumor spread, differing not only in clinical appearance, but also in molecular characteristics and outcome.. EMT, peritoneal inflammation status, and therapeutic options are discussed. SIGNIFICANCE: More than half of serous epithelial ovarian cancer patients present with a newly described type of intraperitoneal tumor spread, associated with differences in the inflammation status, activated oncogenic pathways, lack of EMT, and thus reduced overall survival. Both, the diminished immune reaction and the enhanced epithelial and malignant characteristics of the tumor cells open new avenues for therapeutic options and strategies, like Catumaxomab, already in clinical use.
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spelling pubmed-46273062015-12-02 Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome Auer, Katharina Bachmayr-Heyda, Anna Aust, Stefanie Sukhbaatar, Nyamdelger Reiner, Agnes Teresa Grimm, Christoph Horvat, Reinhard Zeillinger, Robert Pils, Dietmar Oncotarget Research Paper In this study we aimed to analyze the biological mechanisms underlying apparently different modes of peritoneal tumor spread in serous ovarian cancer: miliary (widespread, millet-like lesions) versus non-miliary (bigger, exophytically growing implants). Tumor tissues and ascites from 23 chemotherapy naive patients were analyzed by RNA-sequencing and flow cytometry. On the basis of differential gene expression between miliary and non-miliary, gene signatures were developed. A calculated tumor spread factor revealed a significant independent negative impact of miliary spread on overall survival (HR 3.77; CI(95) 1.14–12.39; p = 0.029) in an independent cohort of 165 serous ovarian cancer patients. Comparing previously published epithelial-mesenchymal transition (EMT) gene signatures, non-miliary spread correlated significantly with a reduced epithelial status. We conclude that serous ovarian cancer is a heterogeneous disease with distinct modes of peritoneal tumor spread, differing not only in clinical appearance, but also in molecular characteristics and outcome.. EMT, peritoneal inflammation status, and therapeutic options are discussed. SIGNIFICANCE: More than half of serous epithelial ovarian cancer patients present with a newly described type of intraperitoneal tumor spread, associated with differences in the inflammation status, activated oncogenic pathways, lack of EMT, and thus reduced overall survival. Both, the diminished immune reaction and the enhanced epithelial and malignant characteristics of the tumor cells open new avenues for therapeutic options and strategies, like Catumaxomab, already in clinical use. Impact Journals LLC 2015-05-11 /pmc/articles/PMC4627306/ /pubmed/25991672 Text en Copyright: © 2015 Auer et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Auer, Katharina
Bachmayr-Heyda, Anna
Aust, Stefanie
Sukhbaatar, Nyamdelger
Reiner, Agnes Teresa
Grimm, Christoph
Horvat, Reinhard
Zeillinger, Robert
Pils, Dietmar
Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title_full Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title_fullStr Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title_full_unstemmed Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title_short Peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
title_sort peritoneal tumor spread in serous ovarian cancer-epithelial mesenchymal status and outcome
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4627306/
https://www.ncbi.nlm.nih.gov/pubmed/25991672
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