The simultaneous loss of Arx and Pax4 genes promotes a somatostatin-producing cell fate specification at the expense of the {alpha}- and {beta}-cell lineages in the mouse endocrine pancreas

doi:10.1242/dev.01870

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Development ePress online publication date 1 Jun 2005
doi: 10.1242/dev.01870

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Research article

The simultaneous loss of Arx and Pax4 genes promotes a somatostatin-producing cell fate specification at the expense of the ${alpha}$ - and ${beta}$ -cell lineages in the mouse endocrine pancreas

Patrick Collombat, Jacob Hecksher-Sørensen, Vania Broccoli, Jens Krull, Ilaria Ponte, Tabea Mundiger, Julian Smith, Peter Gruss, Palle Serup, and Ahmed Mansouri^*
^* Author for correspondence (e-mail: amansou{at}gwdg.de)

The specification of the different mouse pancreatic endocrinesubtypes is determined by the concerted activities of transcriptionfactors. However, the molecular mechanisms regulating endocrinefate allocation remain unclear. In the present study, we uncoverthe molecular consequences of the simultaneous depletion ofArx and Pax4 activity during pancreas development. Our findingsreveal a so far unrecognized essential role of the paired-box-encodingPax4 gene. Specifically, in the combined absence of Arx andPax4, an early-onset loss of mature ${alpha}$ - and ${beta}$ -cells occurs in theendocrine pancreas, concomitantly with a virtually exclusivegeneration of somatostatin-producing cells. Furthermore, despitenormal development of the PP-cells in the double-mutant embryos,an atypical expression of the pancreatic polypeptide (PP) hormonewas observed in somatostatin-labelled cells after birth. Additionalcharacterizations indicate that such an expression of PP wasrelated to the onset of feeding, thereby unravelling an epigeneticcontrol. Finally, our data provide evidence that both Arx andPax4 act as transcriptional repressors that control the expressionlevel of one another, thereby mediating proper endocrine fateallocation.

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				T. Brun and B. R Gauthier A focus on the role of Pax4 in mature pancreatic islet {beta}-cell expansion and survival in health and disease J. Mol. Endocrinol., February 1, 2008; 40(2): 37 - 45. [Abstract] [Full Text] [PDF]

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The simultaneous loss of Arx and Pax4 genes promotes a somatostatin-producing cell fate specification at the expense of the - and -cell lineages in the mouse endocrine pancreas

The simultaneous loss of Arx and Pax4 genes promotes a somatostatin-producing cell fate specification at the expense of the ${alpha}$ - and ${beta}$ -cell lineages in the mouse endocrine pancreas