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Disrupted cell cycle control in cultured endometrial cells from patients with endometriosis harboring the progesterone receptor polymorphism PROGINS. | LitMetric

Disrupted cell cycle control in cultured endometrial cells from patients with endometriosis harboring the progesterone receptor polymorphism PROGINS.

Am J Pathol

Pelvic Pain and Endometriosis Unit, Gynecology Department, Molecular Gynecology and Proteomics Laboratory, Universidade Federal de São Paulo - Escola Paulista de Medicina, São Paulo, Brasil.

Published: July 2009

AI Article Synopsis

  • Endometriosis development and maintenance remain unclear, especially regarding genetic factors like the PROGINS polymorphism in the progesterone receptor gene.
  • A study examined endometrial cells from women with and without endometriosis, revealing that those with the PROGINS allele had increased cell proliferation and viability, along with decreased apoptosis after progesterone treatment.
  • The findings suggest that the PROGINS polymorphism reduces progesterone responsiveness in endometriosis cases, thus potentially exacerbating the disease's symptoms and progression.

Article Abstract

Presently, little is understood about how endometriosis is established or maintained, or how genetic factors can predispose women to the disease. Because of the crucial role that the progesterone receptor polymorphism PROGINS plays in predisposing women to the development of endometriosis, we hypothesized that this variant may influence critical steps during endometrial cell metabolism that are involved in the pathogenesis of endometriosis. Eutopic endometria were collected from three sources: women with endometriosis who had a single PROGINS allele (from the progesterone receptor gene); women with endometriosis who had the wild-type progesterone receptor allele; and women without endometriosis who had the wild-type allele. Cells prepared from the eutopic endometria of these women were stimulated with both estradiol and progesterone, and then examined for cell proliferation, viability, and apoptosis. The cells from women with endometriosis that carried the PROGINS allele demonstrated increased proliferation, greater viability, and decreased apoptosis following progesterone treatment. In general, these parameters were very different as compared with those of women with endometriosis but without the PROGINS allele and women in the control group. This result indicates there is a reduced level of progesterone responsiveness in women who carry the PROGINS polymorphism. Because progesterone responsiveness is known to be an important characteristic of women with endometriosis, these data support the contention that the PROGINS polymorphism enhances the endometriosis phenotype.

Download full-text PDF

Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2708808PMC
http://dx.doi.org/10.2353/ajpath.2009.080966DOI Listing

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