Literature DB >> 28772022

FUCCI tracking shows cell-cycle-dependent Neurog3 variation in pancreatic progenitors.

Matthew E Bechard1, Eric D Bankaitis1, Alessandro Ustione2, David W Piston2, Mark A Magnuson1,2, Christopher V E Wright1.   

Abstract

During pancreas organogenesis, Neurog3HI endocrine-committing cells are generated from a population of Sox9+ mitotic progenitors with only a low level of Neurog3 transcriptional activity (Neurog3TA.LO ). Low-level Neurog3 protein, in Neurog3TA.LO cells, is required to maintain their mitotic endocrine-lineage-primed status. Herein, we describe a Neurog3-driven FUCCI cell-cycle reporter (Neurog3P2A.FUCCI ) derived from a Neurog3 BAC transgenic reporter that functions as a loxed cassette acceptor (LCA). In cycling Sox9+ Neurog3TA.LO progenitors, the majority of cells in S-G2 -M phases have undetectable levels of Neurog3 with increased expression of endocrine progenitor markers, while those in G1 have low Neurog3 levels with increased expression of endocrine differentiation markers. These findings support a model in which variations in Neurog3 protein levels are coordinated with cell-cycle phase progression in Neurog3TA.LO progenitors with entrance into G1 triggering a concerted effort, beyond increasing Neurog3 levels, to maintain an endocrine-lineage-primed state by initiating expression of the downstream endocrine differentiation program prior to endocrine-commitment.
© 2017 Wiley Periodicals, Inc.

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Keywords:  endocrine-biased; lineage priming; progenitor

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Year:  2017        PMID: 28772022      PMCID: PMC5750046          DOI: 10.1002/dvg.23050

Source DB:  PubMed          Journal:  Genesis        ISSN: 1526-954X            Impact factor:   2.487


  23 in total

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  1 in total

1.  Endocrine lineage biases arise in temporally distinct endocrine progenitors during pancreatic morphogenesis.

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Journal:  Nat Commun       Date:  2018-08-22       Impact factor: 14.919

  1 in total

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