FOXO1 and c-jun transcription factors mRNA are modulated in endometriosis

doi:10.1093/molehr/gah119

Mol. Hum. Reprod. Advance Access published online on October 22, 2004
Molecular Human Reproduction, doi:10.1093/molehr/gah119
© 2004 by Oxford University Press

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Received September 8, 2004
Accepted October 4, 2004

Article

FOXO1 and c-jun transcription factors mRNA are modulated in endometriosis

K. Shazand ¹, S. Baban ¹, C. Privé ¹, B. Malette ¹, P. Croteau ¹, M. Lagacé ¹, J.-B. Racine ¹, and P. Hugo ¹^*

¹ Metriogene Biosciences, Inc., Molecular Biology Unit, 6100, Royalmount Ave, Montreal, Quebec, Canada, H4P 2R2

^* To whom correspondence should be addressed.
P. Hugo, E-mail: phugo{at}caprion.com

Abstract

Endometriosis is a polygenic gynaecological condition affecting5-15% of women of childbearing age. Major symptoms of the diseaseare pelvic pain and infertility. No clear link has been establishedbetween symptoms and the stage of the disease. Although someaspects have begun to be clarified, clinical understanding ofendometriosis remains partial at the molecular level. In thisperspective, we targeted isolation of differentially expressedgenes in the eutopic endometrial tissue. Our assumption wasthat the endometrial cells of patients presented an unusualgene expression profile, allowing their implantation and survivalin an ectopic site, leading to endometriotic lesions. Here,we report that mRNA steady-state levels of two key transcriptionfactors are modulated in endometriosis. FOXO1 (also known asFKHR) levels were 1.6-fold lower in endometriosis compared tothe control group at the onset of the secretory phase (day 15-21),while c-jun mRNA was present at higher amounts in endometriosis(1.5-fold) at the proliferative phase of the menstrual cycle.These results were derived from a large sample composed of 157control subjects and 209 patients with endometriosis. Gene profilingwas conducted by real-time quantitative PCR, and data were qualitycontrolled before statistical analysis. Whether protein levelsare affected as well remains to be investigated.

Keywords: c-jun; differential display; endometriosis; FOXO1.

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