Ngn3+ endocrine progenitor cells control the fate and morphogenesis of pancreatic ductal epithelium

Judith Magenheim; Allon M. Klein; Ben Z. Stanger; Ruth Ashery-Padan; Beatriz Sosa-Pineda; Guoqiang Gu; Yuval Dor

doi:https://doi.org/10.1016/j.ydbio.2011.08.006

Ngn3⁺ endocrine progenitor cells control the fate and morphogenesis of pancreatic ductal epithelium

Judith Magenheim, Allon M. Klein, Ben Z. Stanger, Ruth Ashery-Padan, Beatriz Sosa-Pineda, Guoqiang Gu, Yuval Dor

The Hebrew University of Jerusalem, Tel Aviv University

Research output: Contribution to journal › Article › peer-review

Abstract

During pancreas development, endocrine and exocrine cells arise from a common multipotent progenitor pool. How these cell fate decisions are coordinated with tissue morphogenesis is poorly understood. Here we have examined ductal morphology, endocrine progenitor cell fate and Notch signaling in Ngn3^-/- mice, which do not produce islet cells. Ngn3 deficiency results in reduced branching and enlarged pancreatic duct-like structures, concomitant with Ngn3 promoter activation throughout the ductal epithelium and reduced Notch signaling. Conversely, forced generation of surplus endocrine progenitor cells causes reduced duct caliber and an excessive number of tip cells. Thus, endocrine progenitor cells normally provide a feedback signal to adjacent multipotent ductal progenitor cells that activates Notch signaling, inhibits further endocrine differentiation and promotes proper morphogenesis. These results uncover a novel layer of regulation coordinating pancreas morphogenesis and endocrine/exocrine differentiation, and suggest ways to enhance the yield of beta cells from stem cells.

Original language	English
Pages (from-to)	26-36
Number of pages	11
Journal	Developmental Biology
Volume	359
Issue number	1
DOIs	https://doi.org/10.1016/j.ydbio.2011.08.006
State	Published - 1 Nov 2011

Keywords

Branching morphogenesis
Jagged1
Lateral inhibition
Lineage tracing
Neurogenin3
Notch
Pancreas development

All Science Journal Classification (ASJC) codes

Molecular Biology
Developmental Biology
Cell Biology

Access to Document

https://doi.org/10.1016/j.ydbio.2011.08.006

Cite this

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title = "Ngn3+ endocrine progenitor cells control the fate and morphogenesis of pancreatic ductal epithelium",

abstract = "During pancreas development, endocrine and exocrine cells arise from a common multipotent progenitor pool. How these cell fate decisions are coordinated with tissue morphogenesis is poorly understood. Here we have examined ductal morphology, endocrine progenitor cell fate and Notch signaling in Ngn3-/- mice, which do not produce islet cells. Ngn3 deficiency results in reduced branching and enlarged pancreatic duct-like structures, concomitant with Ngn3 promoter activation throughout the ductal epithelium and reduced Notch signaling. Conversely, forced generation of surplus endocrine progenitor cells causes reduced duct caliber and an excessive number of tip cells. Thus, endocrine progenitor cells normally provide a feedback signal to adjacent multipotent ductal progenitor cells that activates Notch signaling, inhibits further endocrine differentiation and promotes proper morphogenesis. These results uncover a novel layer of regulation coordinating pancreas morphogenesis and endocrine/exocrine differentiation, and suggest ways to enhance the yield of beta cells from stem cells.",

keywords = "Branching morphogenesis, Jagged1, Lateral inhibition, Lineage tracing, Neurogenin3, Notch, Pancreas development",

author = "Judith Magenheim and Klein, {Allon M.} and Stanger, {Ben Z.} and Ruth Ashery-Padan and Beatriz Sosa-Pineda and Guoqiang Gu and Yuval Dor",

note = "Funding Information: We thank Abraham Fainsod, Ze'ev Paroush, Klaus Kaestner, Jan Jensen and Palle Serup for stimulating discussions. We thank Maike Sander, Chris Wright and Christoph Kellendonk for generous gifts of Ngn3, Pdx1 and Cre antibodies and Holger Russ for help with dissection of Pax6 mutant embryos. Supported by grants from JDRF , the Helmsley Foundation , the Union Seventh Framework Programme under grant agreement no. 241883 , ERC starting grant and the Dutch Friends of Hebrew University to YD.",

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AU - Magenheim, Judith

AU - Klein, Allon M.

AU - Stanger, Ben Z.

AU - Ashery-Padan, Ruth

AU - Sosa-Pineda, Beatriz

AU - Gu, Guoqiang

AU - Dor, Yuval

N1 - Funding Information: We thank Abraham Fainsod, Ze'ev Paroush, Klaus Kaestner, Jan Jensen and Palle Serup for stimulating discussions. We thank Maike Sander, Chris Wright and Christoph Kellendonk for generous gifts of Ngn3, Pdx1 and Cre antibodies and Holger Russ for help with dissection of Pax6 mutant embryos. Supported by grants from JDRF , the Helmsley Foundation , the Union Seventh Framework Programme under grant agreement no. 241883 , ERC starting grant and the Dutch Friends of Hebrew University to YD.

PY - 2011/11/1

Y1 - 2011/11/1

N2 - During pancreas development, endocrine and exocrine cells arise from a common multipotent progenitor pool. How these cell fate decisions are coordinated with tissue morphogenesis is poorly understood. Here we have examined ductal morphology, endocrine progenitor cell fate and Notch signaling in Ngn3-/- mice, which do not produce islet cells. Ngn3 deficiency results in reduced branching and enlarged pancreatic duct-like structures, concomitant with Ngn3 promoter activation throughout the ductal epithelium and reduced Notch signaling. Conversely, forced generation of surplus endocrine progenitor cells causes reduced duct caliber and an excessive number of tip cells. Thus, endocrine progenitor cells normally provide a feedback signal to adjacent multipotent ductal progenitor cells that activates Notch signaling, inhibits further endocrine differentiation and promotes proper morphogenesis. These results uncover a novel layer of regulation coordinating pancreas morphogenesis and endocrine/exocrine differentiation, and suggest ways to enhance the yield of beta cells from stem cells.

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