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Publication : Single cell RNA sequencing identifies early diversity of sensory neurons forming via bi-potential intermediates.

First Author  Faure L Year  2020
Journal  Nat Commun Volume  11
Issue  1 Pages  4175
PubMed ID  32826903 Mgi Jnum  J:299733
Mgi Id  MGI:6470217 Doi  10.1038/s41467-020-17929-4
Citation  Faure L, et al. (2020) Single cell RNA sequencing identifies early diversity of sensory neurons forming via bi-potential intermediates. Nat Commun 11(1):4175
abstractText  Somatic sensation is defined by the existence of a diversity of primary sensory neurons with unique biological features and response profiles to external and internal stimuli. However, there is no coherent picture about how this diversity of cell states is transcriptionally generated. Here, we use deep single cell analysis to resolve fate splits and molecular biasing processes during sensory neurogenesis in mice. Our results identify a complex series of successive and specific transcriptional changes in post-mitotic neurons that delineate hierarchical regulatory states leading to the generation of the main sensory neuron classes. In addition, our analysis identifies previously undetected early gene modules expressed long before fate determination although being clearly associated with defined sensory subtypes. Overall, the early diversity of sensory neurons is generated through successive bi-potential intermediates in which synchronization of relevant gene modules and concurrent repression of competing fate programs precede cell fate stabilization and final commitment.
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