Exposure of fallopian tube epithelium to follicular fluid mimics carcinogenic changes in precursor lesions of serous papillary carcinoma

K. Bahar-Shany, H. Brand, S. Sapoznik, J. Jacob-Hirsch, Y. Yung, J. Korach, T. Perri, Y. Cohen, A. Hourvitz, K. Levanon

Research output: Contribution to journalArticlepeer-review

82 Scopus citations

Abstract

Objectives Ovulation-related inflammation is suspected to have a causal role in ovarian carcinogenesis, but there are no human models to study the molecular pathways. Our aim is to develop such an ex-vivo model based on human fallopian tube (FT) epithelium exposed to human follicular fluid (FF). Methods FT epithelium was dissociated from normal surgical specimens. FF was obtained from donors undergoing in-vitro fertilization. The cells were cultured on collagen-coated Transwells and incubated with FF for various periods of time. The transcriptomic changes resulting from FF treatment were profiled using Affymetrix expression arrays. Specific characteristics of the FT pre-cancerous lesions were studied using immunohistochemistry, immunofluorescence, RT-PCR and XTT assay. Results We show that FF exposure causes up-regulation of inflammatory and DNA repair pathways. Double stranded DNA breaks are induced. There is a minor increase in cell proliferation. TP53, which is the hallmark of the precursor lesion in-vivo, is accumulated. Levels of expression and secretion of Interleukin-8 are significantly increased. Conclusions Our model addresses the main non-genetic risk factor for ovarian cancer, namely the impact of ovulation. This study demonstrates the biological implications of in-vitro exposure of human FT epithelial cells to FF. The model replicates elements characterizing the precursor lesions of ovarian cancer, and warrants further investigation of the linkage between repeated exposure to ovulation-related damage and accumulation of neoplastic changes.

Original languageEnglish
Pages (from-to)322-327
Number of pages6
JournalGynecologic Oncology
Volume132
Issue number2
DOIs
StatePublished - Feb 2014
Externally publishedYes

Bibliographical note

Funding Information:
This work was supported by research grants from the AACR-George and Patricia Sehl Fellowship for Cancer Genetics Research , the Israel Science Foundation Legacy Heritage Clinical Research Initiative , the Israel Cancer Research Fund Clinical Research Career Development Award , The Israeli Cancer Association , and the Chaim Sheba Medical Center Dr. Pinchas Bornstein Talpiot Medical Leadership Program . None of the funding agencies had any influence on the design of this research or the content of this manuscript. We thank Dr. Ronny Drapkin for kindly sharing with us immortalized FT epithelial cell lines.

Funding

This work was supported by research grants from the AACR-George and Patricia Sehl Fellowship for Cancer Genetics Research , the Israel Science Foundation Legacy Heritage Clinical Research Initiative , the Israel Cancer Research Fund Clinical Research Career Development Award , The Israeli Cancer Association , and the Chaim Sheba Medical Center Dr. Pinchas Bornstein Talpiot Medical Leadership Program . None of the funding agencies had any influence on the design of this research or the content of this manuscript. We thank Dr. Ronny Drapkin for kindly sharing with us immortalized FT epithelial cell lines.

FundersFunder number
AACR-George
Chaim Sheba Medical Center
Israeli Cancer Association
Israel Cancer Research Fund
Israel Science Foundation

    Keywords

    • Biomarkers
    • Carcinogenesis
    • Fallopian tube
    • Follicular fluid
    • Ovarian cancer
    • Ovulation

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