CaltechAUTHORS
Published December 11, 2020 | Version Supplemental Material + Submitted + Accepted Version
Journal Article Open

Developmental clock and mechanism of de novo polarization of the mouse embryo

Creators

  • 1. ROR icon University of Cambridge
  • 2. ROR icon California Institute of Technology
  • 3. ROR icon Tsinghua University

Abstract

Embryo polarization is critical for mouse development; however, neither the regulatory clock nor the molecular trigger that it activates is known. Here, we show that the embryo polarization clock reflects the onset of zygotic genome activation, and we identify three factors required to trigger polarization. Advancing the timing of transcription factor AP-2 gamma (Tfap2c) and TEA domain transcription factor 4 (Tead4) expression in the presence of activated Ras homolog family member A (RhoA) induces precocious polarization as well as subsequent cell fate specification and morphogenesis. Tfap2c and Tead4 induce expression of actin regulators that control the recruitment of apical proteins on the membrane, whereas RhoA regulates their lateral mobility, allowing the emergence of the apical domain. Thus, Tfap2c, Tead4, and RhoA are regulators for the onset of polarization and cell fate segregation in the mouse.

Additional Information

© 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works https://www.sciencemag.org/about/science-licenses-journal-article-reuse. This is an article distributed under the terms of the Science Journals Default License. Received for publication June 10, 2020. Accepted for publication October 14, 2020. We thank E. Munro, D. Glover, A. Andersen, and M. Shahbazi for helpful discussion; S. Shadkhoo for comments on the model; and S. Malas for the Gata3-GFP transgenic line. Some of the computations were conducted on the Caltech High Performance Cluster, supported by a Gordon and Betty Moore Foundation grant. This work was supported by grants from the Wellcome Trust (098287/Z/12/Z), ERC (669198), Leverhulme Trust (RPG-2018-085), Open Philanthropy/Silicon Valley, Weston Havens Foundations and NIH R01 HD100456-01A1 to M.Z.-G; Packard Foundation, Heritage Medical Research Institute, NIH U01CA244109 to M.T.; and the National Key R&D Program of China grants 2017YFA0102802 and 2019YFA0110001 to J.N. Author contributions: Conceptualization: M.Z. and M.Z.-G. Investigation: M.Z., J.C.-S., P.W., and C.E.H. Writing: M.Z. and M.Z.-G. Supervision: M.Z.-G., M.T., and J.N. The authors declare no competing interests. Data and materials availability: All raw data are available upon request from the corresponding author. The RNA-seq data have been deposited in the Gene Expression Omnibus database (accession number GSE124755). The code for computation simulation has been deposited at https://jakesorel.github.io/Apical_Domain_2020/.

Attached Files

Accepted Version - nihms-1714014.pdf

Submitted - 2020.02.10.942201v1.full.pdf

Supplemental Material - abd2703_MDAR_Reproducibility_Checklist.pdf

Supplemental Material - abd2703_Zhu_SM.pdf

Supplemental Material - abd2703s1.mov

Supplemental Material - abd2703s10.mov

Supplemental Material - abd2703s11.mov

Supplemental Material - abd2703s12.mov

Supplemental Material - abd2703s13.mov

Supplemental Material - abd2703s14.mov

Supplemental Material - abd2703s15.mov

Supplemental Material - abd2703s2.mov

Supplemental Material - abd2703s3.mov

Supplemental Material - abd2703s4.mov

Supplemental Material - abd2703s5.mov

Supplemental Material - abd2703s6.mov

Supplemental Material - abd2703s7.mov

Supplemental Material - abd2703s8.mov

Supplemental Material - abd2703s9.mov

Files

nihms-1714014.pdf

Files (140.2 MB)

Name Size Download all
md5:c975986bb36336f8e8bebf91155344fc
25.0 MB Preview Download
md5:71a954d0b6c8373f61c9e0886aaef5a3
101.6 kB Preview Download
md5:cd1dc9727a2ea723765f7c23d84e10fd
19.5 MB Preview Download
md5:6508cd6442981afb625bb11d3c10eb11
5.9 MB Download
md5:e04469707dc78b4caebc994b09cc64bf
3.4 MB Download
md5:13d526f6d483167d226fa89f8e8ccc00
5.3 MB Download
md5:087990d3c95684a3c27a1758374fa11d
13.8 MB Download
md5:a293a7bb3cfb33f861db2a9f787c419f
10.7 MB Download
md5:e297ef0bdd19a48aa99d04142bf62252
8.9 MB Download
md5:7cc6a852fb18045268f78f42955d8d44
5.0 MB Download
md5:2ab90ee6d4c6233868758667c96e172f
5.5 MB Download
md5:d37e277a11ff2d46dade877ab1b2eaf7
2.1 MB Download
md5:f08da9b95b5df803d0efd5e1bb053678
643.7 kB Download
md5:ac1c4dfdd7d090739c8db84343f694b2
502.2 kB Download
md5:be56afba2d074c16089fbdbd241d58af
785.3 kB Download
md5:5492d89b0b75af780fbde0f1f8828f82
10.8 MB Download
md5:d834cf7f9364752f2dd02ae2586bab7b
9.6 MB Download
md5:d7502d329c68e47a5b13da0bc2dadee7
8.8 MB Download
md5:91dc5149b25d73ceef9ac6a159ebfa9a
3.7 MB Preview Download

Additional details

Additional titles

Alternative title
Transcriptional control of apical protein clustering drives de novo cell polarity establishment in the early mouse embryo

Identifiers

PMCID
PMC8210885
Eprint ID
101233
Resolver ID
CaltechAUTHORS:20200212-084819179

Related works

Describes
https://jakesorel.github.io/Apical_Domain_2020/ (URL)
10.1101/2020.02.10.942201 (DOI)

Funding

Gordon and Betty Moore Foundation
Wellcome Trust
098287/Z/12/Z
European Research Council (ERC)
669198
Leverhulme Trust
RPG-2018-085
Open Philanthropy
Weston Havens Foundation
NIH
R01 HD100456-01A1
David and Lucile Packard Foundation
Heritage Medical Research Institute
NIH
U01CA244109
National Key Research and Development Program of China
2017YFA0102802
National Key Research and Development Program of China
2019YFA0110001

Dates

Created
2020-02-12
Created from EPrint's datestamp field
Updated
2023-07-18
Created from EPrint's last_modified field

Caltech Custom Metadata

Caltech groups
Division of Biology and Biological Engineering (BBE), Division of Biology and Biological Engineering (BBE)