Literature DB >> 28854867

An Embryonic and Induced Pluripotent Stem Cell Model for Ovarian Granulosa Cell Development and Steroidogenesis.

Shane Lipskind1, Jennifer S Lindsey1, Behzad Gerami-Naini2, Jennifer L Eaton2, Daniel O'Connell2, Adam Kiezun3, Joshua W K Ho4, Nicholas Ng1, Parveen Parasar1, Michelle Ng1, Michael Nickerson1, Utkan Demirci5, Richard Maas2,6, Raymond M Anchan1,6.   

Abstract

Embryoid bodies (EBs) can serve as a system for evaluating pluripotency, cellular differentiation, and tissue morphogenesis. In this study, we use EBs derived from mouse embryonic stem cells (mESCs) and human amniocyte-derived induced pluripotent stem cells (hAdiPSCs) as a model for ovarian granulosa cell (GC) development and steroidogenic cell commitment. We demonstrated that spontaneously differentiated murine EBs (mEBs) and human EBs (hEBs) displayed ovarian GC markers, such as aromatase (CYP19A1), FOXL2, AMHR2, FSHR, and GJA1. Comparative microarray analysis identified both shared and unique gene expression between mEBs and the maturing mouse ovary. Gene sets related to gonadogenesis, lipid metabolism, and ovarian development were significantly overrepresented in EBs. Of the 29 genes, 15 that were differentially regulated in steroidogenic mEBs displayed temporal expression changes between embryonic, postnatal, and mature ovarian tissues by polymerase chain reaction. Importantly, both mEBs and hEBs were capable of gonadotropin-responsive estradiol (E2) synthesis in vitro (217-759 pg/mL). Live fluorescence-activated cell sorting-sorted AMHR2+ granulosa-like cells from mEBs continued to produce E2 after purification (15.3 pg/mL) and secreted significantly more E2 than AMHR2- cells (8.6 pg/mL, P < .05). We conclude that spontaneously differentiated EBs of both mESC and hAdiPSC origin can serve as a biologically relevant model for ovarian GC differentiation and steroidogenic cell commitment. These cells should be further investigated for therapeutic uses, such as stem cell-based hormone replacement therapy and in vitro maturation of oocytes.

Entities:  

Keywords:  embryonic stem cells; iPSC; native hormones; ovarian tissue regeneration; steroidogenesis

Mesh:

Substances:

Year:  2017        PMID: 28854867      PMCID: PMC6344958          DOI: 10.1177/1933719117725814

Source DB:  PubMed          Journal:  Reprod Sci        ISSN: 1933-7191            Impact factor:   3.060


  50 in total

Review 1.  Sex steroid biosynthesis in white adipose tissue.

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Journal:  Horm Metab Res       Date:  2002 Nov-Dec       Impact factor: 2.936

2.  Menopausal estrogen and estrogen-progestin replacement therapy and breast cancer risk.

Authors:  C Schairer; J Lubin; R Troisi; S Sturgeon; L Brinton; R Hoover
Journal:  JAMA       Date:  2000-01-26       Impact factor: 56.272

3.  Derivation of oocytes from mouse embryonic stem cells.

Authors:  Karin Hübner; Guy Fuhrmann; Lane K Christenson; James Kehler; Rolland Reinbold; Rabindranath De La Fuente; Jennifer Wood; Jerome F Strauss; Michele Boiani; Hans R Schöler
Journal:  Science       Date:  2003-05-01       Impact factor: 47.728

4.  Trophoblast differentiation in embryoid bodies derived from human embryonic stem cells.

Authors:  Behzad Gerami-Naini; Oksana V Dovzhenko; Maureen Durning; Frederick H Wegner; James A Thomson; Thaddeus G Golos
Journal:  Endocrinology       Date:  2003-12-18       Impact factor: 4.736

5.  Ovarian failure after adjuvant chemotherapy is associated with rapid bone loss in women with early-stage breast cancer.

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Journal:  J Clin Oncol       Date:  2001-07-15       Impact factor: 44.544

6.  Effect of hormone replacement therapy on breast cancer risk: estrogen versus estrogen plus progestin.

Authors:  R K Ross; A Paganini-Hill; P C Wan; M C Pike
Journal:  J Natl Cancer Inst       Date:  2000-02-16       Impact factor: 13.506

Review 7.  Adipose tissue intracrinology: potential importance of local androgen/estrogen metabolism in the regulation of adiposity.

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9.  Menopausal hormone replacement therapy and risk of ovarian cancer.

Authors:  James V Lacey; Pamela J Mink; Jay H Lubin; Mark E Sherman; Rebecca Troisi; Patricia Hartge; Arthur Schatzkin; Catherine Schairer
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10.  Foxl2 disruption causes mouse ovarian failure by pervasive blockage of follicle development.

Authors:  Manuela Uda; Chris Ottolenghi; Laura Crisponi; Jose Elias Garcia; Manila Deiana; Wendy Kimber; Antonino Forabosco; Antonio Cao; David Schlessinger; Giuseppe Pilia
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6.  Identification of Hypoxia Signature to Assess the Tumor Immune Microenvironment and Predict Prognosis in Patients with Ovarian Cancer.

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