6533b85afe1ef96bd12b8a14
RESEARCH PRODUCT
false
subject
0301 basic medicineeducation.field_of_studyMesodermPopulationGerm layerBiologyCell fate determinationEmbryonic stem cellCell biologyGastrulation03 medical and health sciences030104 developmental biologymedicine.anatomical_structureSomitogenesismedicineCompartment (development)educationMolecular BiologyDevelopmental Biologydescription
During gastrulation, embryonic cells become specified into distinct germ layers. In mouse, this continues throughout somitogenesis from a population of bipotent stem cells called neuromesodermal progenitors (NMps). However, the degree of self-renewal associated with NMps in the fast-developing zebrafish embryo is unclear. With a genetic clone tracing method, we labelled early embryonic progenitors and find a strong clonal similarity between spinal cord and mesoderm tissues. We followed individual cell lineages by light-sheet imaging, revealing a common neuromesodermal lineage contribution to a subset of spinal cord tissue across the anterior-posterior body axis. An initial population subdivides at mid gastrula stages and is directly allocated to neural and mesodermal compartments during gastrulation. A second population in the tailbud undergoes delayed allocation to contribute to the neural and mesodermal compartment only at late somitogenesis. Cell tracking and retrospective cell fate assignment at late somitogenesis stages reveal these cells to be a collection of mono-fated progenitors. Our results suggest that NMps are a conserved population of bipotential progenitors, whose lineage varies in a species-specific manner due to vastly different rates of differentiation and growth.
| year | journal | country | edition | language |
|---|---|---|---|---|
| 2018-01-01 | Development |