Gata3 regulates trophoblast development downstream of Tead4 and in parallel to Cdx2

Author:

Ralston Amy12,Cox Brian J.1,Nishioka Noriyuki3,Sasaki Hiroshi3,Chea Evelyn1,Rugg-Gunn Peter1,Guo Guoji45,Robson Paul45,Draper Jonathan S.6,Rossant Janet1

Affiliation:

1. Program in Developmental and Stem Cell Biology, Hospital for Sick Children Research Institute, MARS Building, Toronto Medical Discovery Tower, 101 College St, Toronto, ON M5G 1L7, Canada

2. Department of Molecular, Cell, and Developmental Biology, University of California, Santa Cruz, CA 95064, USA

3. Laboratory for Embryonic Induction, RIKEN Center for Developmental Biology, 2-2-3 Minatojima-minamimachi, Chuo-ku, Kobe, Hyogo 650-0047, Japan

4. Department of Biological Sciences, National University of Singapore, Singapore 117543

5. Stem Cell and Developmental Biology, Genome Institute of Singapore, 138672 Singapore

6. McMaster Stem Cell and Cancer Research Institute, 1200 Main Street West, MDCL 5032, Hamilton, ON L8N 3Z5, Canada

Abstract

The mouse blastocyst and stem cells derived from its tissue lineages provide a unique genetic system for examining the establishment and loss of pluripotency. The transcription factor Cdx2 plays a central role by repressing pluripotency genes, such as Oct4, and promoting extraembryonic trophoblast fate at the blastocyst stage. However, genetic evidence has suggested that Cdx2 does not work alone in the trophoblast lineage. We have used bioinformatic and functional genomic strategies to identify the transcription factor Gata3 as a trophoblast factor. We show Gata3 to be capable of inducing trophoblast fate in embryonic stem cells and driving trophoblast differentiation in trophoblast stem cells. In addition, Cdx2 is not required for Gata3-induced expression of a subset of trophoblast genes in embryonic stem cells. We show that Gata3 is coexpressed with Cdx2 in the blastocyst, but this does not depend on Cdx2. In the embryo, expression of Gata3, like that of Cdx2, depends on Tead4, and the expression of both factors becomes restricted to trophoblast by a mechanism that does not initially rely on Oct4. These observations suggest that Gata3 and Cdx2 can act in parallel pathways downstream of Tead4 to induce the expression of common and independent targets in the trophoblast lineage, whereas Oct4 is required for continued repression of trophoblast fate in the embryonic lineage.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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