Literature DB >> 15063174

Zebrafish mnx genes in endocrine and exocrine pancreas formation.

Björn Wendik1, Esther Maier, Dirk Meyer.   

Abstract

The pancreas consists of two components, which exert distinct homeostatic function, an endocrine part that secretes hormones including insulin and an exocrine part that produces digestive enzymes. In mouse, one of the factors essential for development of the pancreas is the Mnx-class homeobox transcription factor Hb9. Genetic studies showed that Hb9 is required for both initial morphogenesis of the pancreas as well as subsequent differentiation of insulin-producing beta-cells [Nat. Genet. 23 (1999) 71; Nat. Genet. 23 (1999) 67]. To get a better understanding of what role mnx genes play in pancreas development, we isolated and characterized mnx genes in the model organism zebrafish. We found one gene with homology to hb9 orthologs and two that display homology to the related chicken mnr2. Embryonic expression of the zebrafish mnx genes is very dynamic and is detected in derivatives of all three germ layers. Endodermal expression of hb9 takes place in the early gut endoderm and, later, in the endocrine pancreas and the swim bladder. In addition, one of the mnr2 genes, mnr2a, shows expression in an endodermal cell population that is initially intermingled with insulin-positive cells and that later becomes restricted to the exocrine pancreas. In knockdown studies using antisense morpholinos, we show that hb9 is essential for differentiation of the insulin-producing beta-cells but unlike mouse Hb9 is not needed for early morphogenesis of the pancreas. In contrast, mnr2a is required during late morphogenesis of the exocrine pancreas. In summary, our data suggest a tissue-specific mnx-expression code in the zebrafish pancreas and they reveal a novel role of an mnr2-related gene.

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Year:  2004        PMID: 15063174     DOI: 10.1016/j.ydbio.2003.12.026

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  25 in total

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Authors:  Burcu Guner; Rolf O Karlstrom
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2.  Loss of function of def selectively up-regulates Delta113p53 expression to arrest expansion growth of digestive organs in zebrafish.

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3.  Zebrafish mnx1 controls cell fate choice in the developing endocrine pancreas.

Authors:  Gokhan Dalgin; Andrea B Ward; Le T Hao; Christine E Beattie; Alexei Nechiporuk; Victoria E Prince
Journal:  Development       Date:  2011-11       Impact factor: 6.868

4.  Specified neural progenitors sort to form sharp domains after noisy Shh signaling.

Authors:  Fengzhu Xiong; Andrea R Tentner; Peng Huang; Arnaud Gelas; Kishore R Mosaliganti; Lydie Souhait; Nicolas Rannou; Ian A Swinburne; Nikolaus D Obholzer; Paul D Cowgill; Alexander F Schier; Sean G Megason
Journal:  Cell       Date:  2013-04-25       Impact factor: 41.582

5.  Mnx1: a gatekeeper of β cell fate.

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Journal:  Islets       Date:  2012-07-01       Impact factor: 2.694

6.  Long-range gene regulation links genomic type 2 diabetes and obesity risk regions to HHEX, SOX4, and IRX3.

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Review 7.  On the diabetic menu: zebrafish as a model for pancreas development and function.

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Journal:  Bioessays       Date:  2009-02       Impact factor: 4.345

8.  Nutrient excess stimulates β-cell neogenesis in zebrafish.

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9.  DEAD-box protein Ddx46 is required for the development of the digestive organs and brain in zebrafish.

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Journal:  PLoS One       Date:  2012-03-19       Impact factor: 3.240

10.  Cellular dissection of the spinal cord motor column by BAC transgenesis and gene trapping in zebrafish.

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Journal:  Front Neural Circuits       Date:  2013-05-28       Impact factor: 3.492

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