In Vitro Modeling of Human Germ Cell Development Using Pluripotent Stem Cells

  • Yuncheng Zhao
  • , Shicheng Ye
  • , Dongli Liang
  • , Pengxiang Wang
  • , Jing Fu
  • , Qing Ma
  • , Ruijiao Kong
  • , Linghong Shi
  • , Xueping Gong
  • , Wei Chen
  • , Wubin Ding
  • , Wenjing Yang
  • , Zijue Zhu
  • , Huixing Chen
  • , Xiaoxi Sun
  • , Jun Zhu
  • , Zheng Li
  • , Yuan Wang*
  • *Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

61 Scopus citations

Abstract

Due to differences across species, the mechanisms of cell fate decisions determined in mice cannot be readily extrapolated to humans. In this study, we developed a feeder- and xeno-free culture protocol that efficiently induced human pluripotent stem cells (iPSCs) into PLZF+/GPR125+/CD90+ spermatogonium-like cells (SLCs). These SLCs were enriched with key genes in germ cell development such as MVH, DAZL, GFRα1, NANOS3, and DMRT1. In addition, a small fraction of SLCs went through meiosis in vitro to develop into haploid cells. We further demonstrated that this chemically defined induction protocol faithfully recapitulated the features of compromised germ cell development of PSCs with NANOS3 deficiency or iPSC lines established from patients with non-obstructive azoospermia. Taken together, we established a powerful experimental platform to investigate human germ cell development and pathology related to male infertility. In this article, Wang and colleagues established a feeder- and xeno-free system to robustly induce human pluripotent stem cells (PSCs) into spermatogonia-like cells. This chemically defined induction protocol faithfully recapitulated the features of compromised germ cell development of PSCs with NANOS3 deficiency or iPSC lines established from patients with non-obstructive azoospermia.

Original languageEnglish
Pages (from-to)509-523
Number of pages15
JournalStem Cell Reports
Volume10
Issue number2
DOIs
StatePublished - 13 Feb 2018

Keywords

  • infertility
  • non-obstructive azoospermia
  • pluripotent stem cells
  • spermatogonia

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