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. 2021 May 18;35(7):109138.
doi: 10.1016/j.celrep.2021.109138.

Pluripotent stem cell-derived endometrial stromal fibroblasts in a cyclic, hormone-responsive, coculture model of human decidua

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Pluripotent stem cell-derived endometrial stromal fibroblasts in a cyclic, hormone-responsive, coculture model of human decidua

Virginia Chu Cheung et al. Cell Rep. .
Free article

Abstract

Various human diseases and pregnancy-related disorders reflect endometrial dysfunction. However, rodent models do not share fundamental biological processes with the human endometrium, such as spontaneous decidualization, and no existing human cell cultures recapitulate the cyclic interactions between endometrial stromal and epithelial compartments necessary for decidualization and implantation. Here we report a protocol differentiating human pluripotent stem cells into endometrial stromal fibroblasts (PSC-ESFs) that are highly pure and able to decidualize. Coculture of PSC-ESFs with placenta-derived endometrial epithelial cells generated organoids used to examine stromal-epithelial interactions. Cocultures exhibited specific endometrial markers in the appropriate compartments, organization with cell polarity, and hormone responsiveness of both cell types. Furthermore, cocultures recapitulate a central feature of the human decidua by cyclically responding to hormone withdrawal followed by hormone retreatment. This advance enables mechanistic studies of the cyclic responses that characterize the human endometrium.

Keywords: cell-cell signaling; cyclic hormone response; decidua; decidual stromal cells; endometrial epithelial organoid; endometrial stromal cells; epithelial-stromal signaling; human pluripotent stem cells; uterus.

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Conflict of interest statement

Declaration of interests V.C.C., C.-Y.P., and J.A.K. have filed a provisional patent for the protocol described. M.M., N.J.S., I.A., M.A.N., C.O., and V.J.L. declare no competing interests.

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