A PAX5-OCT4-PRDM1 developmental switch specifies human primordial germ cells

Fang Fang; Benjamin Angulo; Ninuo Xia; Meena Sukhwani; Zhengyuan Wang; Charles C. Carey; Aurélien Mazurie; Jun Cui; Royce Wilkinson; Blake Wiedenheft; Naoko Irie; M. Azim Surani; Kyle E. Orwig; Renee A. Reijo Pera

doi:10.1038/s41556-018-0094-3

A PAX5-OCT4-PRDM1 developmental switch specifies human primordial germ cells

Fang Fang, Benjamin Angulo, Ninuo Xia, Meena Sukhwani, Zhengyuan Wang, Charles C. Carey, Aurélien Mazurie, Jun Cui, Royce Wilkinson, Blake Wiedenheft, Naoko Irie, M. Azim Surani, Kyle E. Orwig, Renee A. Reijo Pera

Research output: Contribution to journal › Article › peer-review

24 Citations (Scopus)

Abstract

Dysregulation of genetic pathways during human germ cell development leads to infertility. Here, we analysed bona fide human primordial germ cells (hPGCs) to probe the developmental genetics of human germ cell specification and differentiation. We examined the distribution of OCT4 occupancy in hPGCs relative to human embryonic stem cells (hESCs). We demonstrated that development, from pluripotent stem cells to germ cells, is driven by switching partners with OCT4 from SOX2 to PAX5 and PRDM1. Gain- and loss-of-function studies revealed that PAX5 encodes a critical regulator of hPGC development. Moreover, an epistasis analysis indicated that PAX5 acts upstream of OCT4 and PRDM1. The PAX5-OCT4-PRDM1 proteins form a core transcriptional network that activates germline and represses somatic programmes during human germ cell differentiation. These findings illustrate the power of combined genome editing, cell differentiation and engraftment for probing human developmental genetics that have historically been difficult to study.

Original language	English
Pages (from-to)	655-665
Number of pages	11
Journal	Nature Cell Biology
Volume	20
Issue number	6
DOIs	https://doi.org/10.1038/s41556-018-0094-3
Publication status	Published - 2018 Jun 1
Externally published	Yes

ASJC Scopus subject areas

Cell Biology

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title = "A PAX5-OCT4-PRDM1 developmental switch specifies human primordial germ cells",

abstract = "Dysregulation of genetic pathways during human germ cell development leads to infertility. Here, we analysed bona fide human primordial germ cells (hPGCs) to probe the developmental genetics of human germ cell specification and differentiation. We examined the distribution of OCT4 occupancy in hPGCs relative to human embryonic stem cells (hESCs). We demonstrated that development, from pluripotent stem cells to germ cells, is driven by switching partners with OCT4 from SOX2 to PAX5 and PRDM1. Gain- and loss-of-function studies revealed that PAX5 encodes a critical regulator of hPGC development. Moreover, an epistasis analysis indicated that PAX5 acts upstream of OCT4 and PRDM1. The PAX5-OCT4-PRDM1 proteins form a core transcriptional network that activates germline and represses somatic programmes during human germ cell differentiation. These findings illustrate the power of combined genome editing, cell differentiation and engraftment for probing human developmental genetics that have historically been difficult to study.",

author = "Fang Fang and Benjamin Angulo and Ninuo Xia and Meena Sukhwani and Zhengyuan Wang and Carey, {Charles C.} and Aur{\'e}lien Mazurie and Jun Cui and Royce Wilkinson and Blake Wiedenheft and Naoko Irie and Surani, {M. Azim} and Orwig, {Kyle E.} and {Reijo Pera}, {Renee A.}",

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AU - Fang, Fang

AU - Angulo, Benjamin

AU - Xia, Ninuo

AU - Sukhwani, Meena

AU - Wang, Zhengyuan

AU - Carey, Charles C.

AU - Mazurie, Aurélien

AU - Cui, Jun

AU - Wilkinson, Royce

AU - Wiedenheft, Blake

AU - Irie, Naoko

AU - Surani, M. Azim

AU - Orwig, Kyle E.

AU - Reijo Pera, Renee A.

PY - 2018/6/1

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N2 - Dysregulation of genetic pathways during human germ cell development leads to infertility. Here, we analysed bona fide human primordial germ cells (hPGCs) to probe the developmental genetics of human germ cell specification and differentiation. We examined the distribution of OCT4 occupancy in hPGCs relative to human embryonic stem cells (hESCs). We demonstrated that development, from pluripotent stem cells to germ cells, is driven by switching partners with OCT4 from SOX2 to PAX5 and PRDM1. Gain- and loss-of-function studies revealed that PAX5 encodes a critical regulator of hPGC development. Moreover, an epistasis analysis indicated that PAX5 acts upstream of OCT4 and PRDM1. The PAX5-OCT4-PRDM1 proteins form a core transcriptional network that activates germline and represses somatic programmes during human germ cell differentiation. These findings illustrate the power of combined genome editing, cell differentiation and engraftment for probing human developmental genetics that have historically been difficult to study.

AB - Dysregulation of genetic pathways during human germ cell development leads to infertility. Here, we analysed bona fide human primordial germ cells (hPGCs) to probe the developmental genetics of human germ cell specification and differentiation. We examined the distribution of OCT4 occupancy in hPGCs relative to human embryonic stem cells (hESCs). We demonstrated that development, from pluripotent stem cells to germ cells, is driven by switching partners with OCT4 from SOX2 to PAX5 and PRDM1. Gain- and loss-of-function studies revealed that PAX5 encodes a critical regulator of hPGC development. Moreover, an epistasis analysis indicated that PAX5 acts upstream of OCT4 and PRDM1. The PAX5-OCT4-PRDM1 proteins form a core transcriptional network that activates germline and represses somatic programmes during human germ cell differentiation. These findings illustrate the power of combined genome editing, cell differentiation and engraftment for probing human developmental genetics that have historically been difficult to study.

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A PAX5-OCT4-PRDM1 developmental switch specifies human primordial germ cells

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