Literature DB >> 25063451

The nuclear hormone receptor family member NR5A2 controls aspects of multipotent progenitor cell formation and acinar differentiation during pancreatic organogenesis.

Michael A Hale1, Galvin H Swift1, Chinh Q Hoang1, Tye G Deering1, Toshi Masui1, Youn-Kyoung Lee2, Jumin Xue1, Raymond J MacDonald3.   

Abstract

The orphan nuclear receptor NR5A2 is necessary for the stem-like properties of the epiblast of the pre-gastrulation embryo and for cellular and physiological homeostasis of endoderm-derived organs postnatally. Using conditional gene inactivation, we show that Nr5a2 also plays crucial regulatory roles during organogenesis. During the formation of the pancreas, Nr5a2 is necessary for the expansion of the nascent pancreatic epithelium, for the subsequent formation of the multipotent progenitor cell (MPC) population that gives rise to pre-acinar cells and bipotent cells with ductal and islet endocrine potential, and for the formation and differentiation of acinar cells. At birth, the NR5A2-deficient pancreas has defects in all three epithelial tissues: a partial loss of endocrine cells, a disrupted ductal tree and a >90% deficit of acini. The acinar defects are due to a combination of fewer MPCs, deficient allocation of those MPCs to pre-acinar fate, disruption of acinar morphogenesis and incomplete acinar cell differentiation. NR5A2 controls these developmental processes directly as well as through regulatory interactions with other pancreatic transcriptional regulators, including PTF1A, MYC, GATA4, FOXA2, RBPJL and MIST1 (BHLHA15). In particular, Nr5a2 and Ptf1a establish mutually reinforcing regulatory interactions and collaborate to control developmentally regulated pancreatic genes by binding to shared transcriptional regulatory regions. At the final stage of acinar cell development, the absence of NR5A2 affects the expression of Ptf1a and its acinar specific partner Rbpjl, so that the few acinar cells that form do not complete differentiation. Nr5a2 controls several temporally distinct stages of pancreatic development that involve regulatory mechanisms relevant to pancreatic oncogenesis and the maintenance of the exocrine phenotype.
© 2014. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  Acinar cell; Mouse; Nr5a2; Organogenesis; Pancreas; Transcriptional control

Mesh:

Substances:

Year:  2014        PMID: 25063451      PMCID: PMC4197540          DOI: 10.1242/dev.109405

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  69 in total

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Journal:  Dev Cell       Date:  2010-06-15       Impact factor: 12.270

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Authors:  Toshihiko Masui; Galvin H Swift; Tye Deering; Chengcheng Shen; Ward S Coats; Qiaoming Long; Hans-Peter Elsässer; Mark A Magnuson; Raymond J MacDonald
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  39 in total

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5.  CONSERVED AND EXAPTED FUNCTIONS OF NUCLEAR RECEPTORS IN ANIMAL DEVELOPMENT.

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6.  MIST1 and PTF1 Collaborate in Feed-Forward Regulatory Loops That Maintain the Pancreatic Acinar Phenotype in Adult Mice.

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7.  Transcriptional Maintenance of Pancreatic Acinar Identity, Differentiation, and Homeostasis by PTF1A.

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