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A single-embryo, single-cell time-resolved model for mouse gastrulation

Mouse embryonic development is a canonical model system for studying mammalian cell fate acquisition. Recently, single-cell atlases comprehensively charted embryonic transcriptional landscapes, yet inference of the coordinated dynamics of cells over such atlases remains challenging. Here, we introdu...

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Autores principales: Mittnenzweig, Markus, Mayshar, Yoav, Cheng, Saifeng, Ben-Yair, Raz, Hadas, Ron, Rais, Yoach, Chomsky, Elad, Reines, Netta, Uzonyi, Anna, Lumerman, Lior, Lifshitz, Aviezer, Mukamel, Zohar, Orenbuch, Ayelet-Hashahar, Tanay, Amos, Stelzer, Yonatan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8162424/
https://www.ncbi.nlm.nih.gov/pubmed/33932341
http://dx.doi.org/10.1016/j.cell.2021.04.004
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author Mittnenzweig, Markus
Mayshar, Yoav
Cheng, Saifeng
Ben-Yair, Raz
Hadas, Ron
Rais, Yoach
Chomsky, Elad
Reines, Netta
Uzonyi, Anna
Lumerman, Lior
Lifshitz, Aviezer
Mukamel, Zohar
Orenbuch, Ayelet-Hashahar
Tanay, Amos
Stelzer, Yonatan
author_facet Mittnenzweig, Markus
Mayshar, Yoav
Cheng, Saifeng
Ben-Yair, Raz
Hadas, Ron
Rais, Yoach
Chomsky, Elad
Reines, Netta
Uzonyi, Anna
Lumerman, Lior
Lifshitz, Aviezer
Mukamel, Zohar
Orenbuch, Ayelet-Hashahar
Tanay, Amos
Stelzer, Yonatan
author_sort Mittnenzweig, Markus
collection PubMed
description Mouse embryonic development is a canonical model system for studying mammalian cell fate acquisition. Recently, single-cell atlases comprehensively charted embryonic transcriptional landscapes, yet inference of the coordinated dynamics of cells over such atlases remains challenging. Here, we introduce a temporal model for mouse gastrulation, consisting of data from 153 individually sampled embryos spanning 36 h of molecular diversification. Using algorithms and precise timing, we infer differentiation flows and lineage specification dynamics over the embryonic transcriptional manifold. Rapid transcriptional bifurcations characterize the commitment of early specialized node and blood cells. However, for most lineages, we observe combinatorial multi-furcation dynamics rather than hierarchical transcriptional transitions. In the mesoderm, dozens of transcription factors combinatorially regulate multifurcations, as we exemplify using time-matched chimeric embryos of Foxc1/Foxc2 mutants. Our study rejects the notion of differentiation being governed by a series of binary choices, providing an alternative quantitative model for cell fate acquisition.
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spelling pubmed-81624242021-06-02 A single-embryo, single-cell time-resolved model for mouse gastrulation Mittnenzweig, Markus Mayshar, Yoav Cheng, Saifeng Ben-Yair, Raz Hadas, Ron Rais, Yoach Chomsky, Elad Reines, Netta Uzonyi, Anna Lumerman, Lior Lifshitz, Aviezer Mukamel, Zohar Orenbuch, Ayelet-Hashahar Tanay, Amos Stelzer, Yonatan Cell Article Mouse embryonic development is a canonical model system for studying mammalian cell fate acquisition. Recently, single-cell atlases comprehensively charted embryonic transcriptional landscapes, yet inference of the coordinated dynamics of cells over such atlases remains challenging. Here, we introduce a temporal model for mouse gastrulation, consisting of data from 153 individually sampled embryos spanning 36 h of molecular diversification. Using algorithms and precise timing, we infer differentiation flows and lineage specification dynamics over the embryonic transcriptional manifold. Rapid transcriptional bifurcations characterize the commitment of early specialized node and blood cells. However, for most lineages, we observe combinatorial multi-furcation dynamics rather than hierarchical transcriptional transitions. In the mesoderm, dozens of transcription factors combinatorially regulate multifurcations, as we exemplify using time-matched chimeric embryos of Foxc1/Foxc2 mutants. Our study rejects the notion of differentiation being governed by a series of binary choices, providing an alternative quantitative model for cell fate acquisition. Cell Press 2021-05-27 /pmc/articles/PMC8162424/ /pubmed/33932341 http://dx.doi.org/10.1016/j.cell.2021.04.004 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Mittnenzweig, Markus
Mayshar, Yoav
Cheng, Saifeng
Ben-Yair, Raz
Hadas, Ron
Rais, Yoach
Chomsky, Elad
Reines, Netta
Uzonyi, Anna
Lumerman, Lior
Lifshitz, Aviezer
Mukamel, Zohar
Orenbuch, Ayelet-Hashahar
Tanay, Amos
Stelzer, Yonatan
A single-embryo, single-cell time-resolved model for mouse gastrulation
title A single-embryo, single-cell time-resolved model for mouse gastrulation
title_full A single-embryo, single-cell time-resolved model for mouse gastrulation
title_fullStr A single-embryo, single-cell time-resolved model for mouse gastrulation
title_full_unstemmed A single-embryo, single-cell time-resolved model for mouse gastrulation
title_short A single-embryo, single-cell time-resolved model for mouse gastrulation
title_sort single-embryo, single-cell time-resolved model for mouse gastrulation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8162424/
https://www.ncbi.nlm.nih.gov/pubmed/33932341
http://dx.doi.org/10.1016/j.cell.2021.04.004
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