Induction of fetal meiotic oocytes from embryonic stem cells in cynomolgus monkeys

Author:

Gyobu‐Motani Sayuri12ORCID,Yabuta Yukihiro12,Mizuta Ken12ORCID,Katou Yoshitaka12,Okamoto Ikuhiro12ORCID,Kawasaki Masanori12ORCID,Kitamura Ayaka12,Tsukiyama Tomoyuki13ORCID,Iwatani Chizuru3,Tsuchiya Hideaki3,Tsujimura Taro1,Yamamoto Takuya145,Nakamura Tomonori126ORCID,Saitou Mitinori124ORCID

Affiliation:

1. Institute for the Advanced Study of Human Biology (WPI‐ASHBi) Kyoto University Kyoto Japan

2. Department of Anatomy and Cell Biology, Graduate School of Medicine Kyoto University Kyoto Japan

3. Research Center for Animal Life Science Shiga University of Medical Science Otsu Japan

4. Center for iPS Cell Research and Application (CiRA) Kyoto University Kyoto Japan

5. Center for Advanced Intelligence Project, RIKEN Tokyo Japan

6. The Hakubi Center for Advanced Research Kyoto University Kyoto Japan

Abstract

AbstractHuman in vitro oogenesis provides a framework for clarifying the mechanism of human oogenesis. To create its benchmark, it is vital to promote in vitro oogenesis using a model physiologically close to humans. Here, we establish a foundation for in vitro oogenesis in cynomolgus (cy) monkeys (Macaca fascicularis): cy female embryonic stem cells harboring one active and one inactive X chromosome (Xa and Xi, respectively) differentiate robustly into primordial germ cell‐like cells, which in xenogeneic reconstituted ovaries develop efficiently into oogonia and, remarkably, further into meiotic oocytes at the zygotene stage. This differentiation entails comprehensive epigenetic reprogramming, including Xi reprogramming, yet Xa and Xi remain epigenetically asymmetric with, as partly observed in vivo, incomplete Xi reactivation. In humans and monkeys, the Xi epigenome in pluripotent stem cells functions as an Xi‐reprogramming determinant. We further show that developmental pathway over‐activations with suboptimal up‐regulation of relevant meiotic genes impede in vitro meiotic progression. Cy in vitro oogenesis exhibits critical homology with the human system, including with respect to bottlenecks, providing a salient model for advancing human in vitro oogenesis.

Funder

Human Frontier Science Program

Japan Society for the Promotion of Science

Exploratory Research for Advanced Technology

Publisher

Springer Science and Business Media LLC

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,Molecular Biology,General Neuroscience

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