Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors

Early in pancreatic development, epithelial cells of pancreatic buds function as primary multipotent progenitor cells (1°MPC) that specify all three pancreatic cell lineages, i.e., endocrine, acinar and duct. Bipotent "Trunk" progenitors derived from 1°MPC are implicated in directly regula...

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Autores principales: Nishimura, Wataru, Kapoor, Archana, El Khattabi, Ilham, Jin, Wanzhu, Yasuda, Kazuki, Bonner-Weir, Susan, Sharma, Arun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4635002/
https://www.ncbi.nlm.nih.gov/pubmed/26540252
http://dx.doi.org/10.1371/journal.pone.0142286
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author Nishimura, Wataru
Kapoor, Archana
El Khattabi, Ilham
Jin, Wanzhu
Yasuda, Kazuki
Bonner-Weir, Susan
Sharma, Arun
author_facet Nishimura, Wataru
Kapoor, Archana
El Khattabi, Ilham
Jin, Wanzhu
Yasuda, Kazuki
Bonner-Weir, Susan
Sharma, Arun
author_sort Nishimura, Wataru
collection PubMed
description Early in pancreatic development, epithelial cells of pancreatic buds function as primary multipotent progenitor cells (1°MPC) that specify all three pancreatic cell lineages, i.e., endocrine, acinar and duct. Bipotent "Trunk" progenitors derived from 1°MPC are implicated in directly regulating the specification of endocrine progenitors. It is unclear if this specification process is initiated in the 1°MPC where some 1°MPC become competent for later specification of endocrine progenitors. Previously we reported that in Pdx1 (tTA/+) ;tetO (MafA) (bigenic) mice inducing expression of transcription factor MafA in Pdx1-expressing (Pdx1(+)) cells throughout embryonic development inhibited the proliferation and differentiation of 1°MPC cells, resulting in reduced pancreatic mass and endocrine cells by embryonic day (E) 17.5. Induction of the transgene only until E12.5 in Pdx1(+) 1°MPC was sufficient for this inhibition of endocrine cells and pancreatic mass at E17.5. However, by birth (P0), as we now report, such bigenic pups had significantly increased pancreatic and endocrine volumes with endocrine clusters containing all pancreatic endocrine cell types. The increase in endocrine cells resulted from a higher proliferation of tubular epithelial cells expressing the progenitor marker Glut2 in E17.5 bigenic embryos and increased number of Neurog3-expressing cells at E19.5. A BrdU-labeling study demonstrated that inhibiting proliferation of 1°MPC by forced MafA-expression did not lead to retention of those progenitors in E17.5 tubular epithelium. Our data suggest that the forced MafA expression in the 1°MPC inhibits their competency to specify endocrine progenitors only until E17.5, and after that compensatory proliferation of tubular epithelium gives rise to a distinct pool of endocrine progenitors. Thus, these bigenic mice provide a novel way to characterize the competency of 1°MPC for their ability to specify endocrine progenitors, a critical limitation in our understanding of endocrine differentiation.
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spelling pubmed-46350022015-11-13 Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors Nishimura, Wataru Kapoor, Archana El Khattabi, Ilham Jin, Wanzhu Yasuda, Kazuki Bonner-Weir, Susan Sharma, Arun PLoS One Research Article Early in pancreatic development, epithelial cells of pancreatic buds function as primary multipotent progenitor cells (1°MPC) that specify all three pancreatic cell lineages, i.e., endocrine, acinar and duct. Bipotent "Trunk" progenitors derived from 1°MPC are implicated in directly regulating the specification of endocrine progenitors. It is unclear if this specification process is initiated in the 1°MPC where some 1°MPC become competent for later specification of endocrine progenitors. Previously we reported that in Pdx1 (tTA/+) ;tetO (MafA) (bigenic) mice inducing expression of transcription factor MafA in Pdx1-expressing (Pdx1(+)) cells throughout embryonic development inhibited the proliferation and differentiation of 1°MPC cells, resulting in reduced pancreatic mass and endocrine cells by embryonic day (E) 17.5. Induction of the transgene only until E12.5 in Pdx1(+) 1°MPC was sufficient for this inhibition of endocrine cells and pancreatic mass at E17.5. However, by birth (P0), as we now report, such bigenic pups had significantly increased pancreatic and endocrine volumes with endocrine clusters containing all pancreatic endocrine cell types. The increase in endocrine cells resulted from a higher proliferation of tubular epithelial cells expressing the progenitor marker Glut2 in E17.5 bigenic embryos and increased number of Neurog3-expressing cells at E19.5. A BrdU-labeling study demonstrated that inhibiting proliferation of 1°MPC by forced MafA-expression did not lead to retention of those progenitors in E17.5 tubular epithelium. Our data suggest that the forced MafA expression in the 1°MPC inhibits their competency to specify endocrine progenitors only until E17.5, and after that compensatory proliferation of tubular epithelium gives rise to a distinct pool of endocrine progenitors. Thus, these bigenic mice provide a novel way to characterize the competency of 1°MPC for their ability to specify endocrine progenitors, a critical limitation in our understanding of endocrine differentiation. Public Library of Science 2015-11-05 /pmc/articles/PMC4635002/ /pubmed/26540252 http://dx.doi.org/10.1371/journal.pone.0142286 Text en © 2015 Nishimura et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Nishimura, Wataru
Kapoor, Archana
El Khattabi, Ilham
Jin, Wanzhu
Yasuda, Kazuki
Bonner-Weir, Susan
Sharma, Arun
Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title_full Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title_fullStr Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title_full_unstemmed Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title_short Compensatory Response by Late Embryonic Tubular Epithelium to the Reduction in Pancreatic Progenitors
title_sort compensatory response by late embryonic tubular epithelium to the reduction in pancreatic progenitors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4635002/
https://www.ncbi.nlm.nih.gov/pubmed/26540252
http://dx.doi.org/10.1371/journal.pone.0142286
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