A Gene Regulatory Network Balances Neural and Mesoderm Specification during Vertebrate Trunk Development

Mina Gouti(Max Delbrück Center), Julien Delile(The Francis Crick Institute), Despina Stamataki(The Francis Crick Institute), Filip J. Wymeersch(MRC Centre for Regenerative Medicine), Yali Huang(MRC Centre for Regenerative Medicine), Jens Kleinjung(The Francis Crick Institute), Valerie Wilson(University of Edinburgh), James Briscoe(The Francis Crick Institute)
Developmental Cell
April 27, 2017
Cited by 287Open Access
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Abstract

Transcriptional networks, regulated by extracellular signals, control cell fate decisions and determine the size and composition of developing tissues. One example is the network controlling bipotent neuromesodermal progenitors (NMPs) that fuel embryo elongation by generating spinal cord and trunk mesoderm tissue. Here, we use single-cell transcriptomics to identify the molecular signature of NMPs and reverse engineer the mechanism that regulates their differentiation. Together with genetic perturbations, this reveals a transcriptional network that integrates opposing retinoic acid (RA) and Wnt signals to determine the rate at which cells enter and exit the NMP state. RA, produced by newly generated mesodermal cells, provides feedback that initiates NMP generation and induces neural differentiation, thereby coordinating the production of neural and mesodermal tissue. Together, the data define a regulatory network architecture that balances the generation of different cell types from bipotential progenitors in order to facilitate orderly axis elongation.


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