Scaffold-free endometrial organoids respond to excess androgens associated with polycystic ovarian syndrome
T Wiwatpanit, AR Murphy, Z Lu… - The Journal of …, 2020 - academic.oup.com
T Wiwatpanit, AR Murphy, Z Lu, M Urbanek, JE Burdette, TK Woodruff, JJ Kim
The Journal of Clinical Endocrinology & Metabolism, 2020•academic.oup.comContext Polycystic ovary syndrome (PCOS) is a prevalent disorder in reproductive aged
women associated with a number of endocrine and metabolic complications, including
increased risk of endometrial cancer. Objective To study the effect of the characteristic
increased androgen levels in PCOS on the endometrium, a novel scaffold-free multicellular
endometrial organoid was established. Design Human endometrial organoids were
constructed using primary endometrial epithelial and stromal cells from endometrial tissues …
women associated with a number of endocrine and metabolic complications, including
increased risk of endometrial cancer. Objective To study the effect of the characteristic
increased androgen levels in PCOS on the endometrium, a novel scaffold-free multicellular
endometrial organoid was established. Design Human endometrial organoids were
constructed using primary endometrial epithelial and stromal cells from endometrial tissues …
Context
Polycystic ovary syndrome (PCOS) is a prevalent disorder in reproductive aged women associated with a number of endocrine and metabolic complications, including increased risk of endometrial cancer.
Objective
To study the effect of the characteristic increased androgen levels in PCOS on the endometrium, a novel scaffold-free multicellular endometrial organoid was established.
Design
Human endometrial organoids were constructed using primary endometrial epithelial and stromal cells from endometrial tissues. Organoids were treated for 14 days with physiologic levels of estradiol and testosterone to mimic a normal follicular phase or PCOS hormone profiles. Organoids were harvested for immunostaining and ribonucleic acid sequencing.
Setting
Academic institution.
Patients
Endometrial tissues from 10 premenopausal women undergoing hysterectomy for benign pathologies were obtained following written consent.
Main Outcome Measures
Organoid architecture, cell specific markers, functional markers, proliferation, and gene expression were measured.
Results
A method to generate scaffold-free endometrial organoids containing epithelial and stromal cells was established. These organoids exhibited distinct organization with epithelial cells lining the outer surface and stromal cells in the center of the organoids. Epithelial cells were polarized, organoids expressed cell type specific and functional markers, as well as androgen, estrogen, and progesterone receptors. Treatment with PCOS hormones increased cell proliferation and dysregulated genes in endometrial organoids.
Conclusions
A new multicellular, scaffold-free endometrial organoid system was established that resembled physiology of the native endometrium. Excess androgens in PCOS promoted cell proliferation in endometrial organoids, revealing new mechanisms of PCOS-associated with risk of endometrial neoplasia.
Oxford University Press