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The mammal-specific Pdx1 Area II enhancer has multiple essential functions in early endocrine cell specification and postnatal β-cell maturation.

Citation
Yang, Y. -P., et al. “The Mammal-Specific Pdx1 Area Ii Enhancer Has Multiple Essential Functions In Early Endocrine Cell Specification And Postnatal Β-Cell Maturation.”. Development (Cambridge, England), pp. 248-257.
Center Vanderbilt University
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Author Yu-Ping Yang, Mark A Magnuson, Roland Stein, Christopher E Wright V
Keywords Cis-regulatory function, Lineage diversification, mouse, Pancreatic endocrine progenitors, Pdx1 enhancer Area II
Abstract

The transcription factor Pdx1 is required for multiple aspects of pancreatic organogenesis. It remains unclear to what extent Pdx1 expression and function depend upon trans-activation through 5' conserved cis-regulatory regions and, in particular, whether the mammal-specific Area II (-2139 to -1958 bp) affects minor or major aspects of organogenesis. We show that Area II is a primary effector of endocrine-selective transcription in epithelial multipotent cells, nascent endocrine progenitors, and differentiating and mature β cells in vivo Pdx1 mice exhibit a massive reduction in endocrine progenitor cells and progeny hormone-producing cells, indicating that Area II activity is fundamental to mounting an effective endocrine lineage-specification program within the multipotent cell population. Creating an Area II-deleted state within already specified Neurog3-expressing endocrine progenitor cells increased the proportion of glucagon α relative to insulin β cells, associated with the transcriptional and epigenetic derepression of the α-cell-determining Arx gene in endocrine progenitors. There were also glucagon and insulin co-expressing cells, and β cells that were incapable of maturation. Creating the Pdx1 state after cells entered an insulin-expressing stage led to immature and dysfunctional islet β cells carrying abnormal chromatin marking in vital β-cell-associated genes. Therefore, trans-regulatory integration through Area II mediates a surprisingly extensive range of progenitor and β-cell-specific Pdx1 functions.

Year of Publication
2017
Journal
Development (Cambridge, England)
Volume
144
Issue
2
Number of Pages
248-257
Date Published
12/2017
ISSN Number
1477-9129
DOI
10.1242/dev.143123
Alternate Journal
Development
PMID
27993987
PMCID
PMC5394757
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