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Publication : The Genetic Program of Pancreatic β-Cell Replication In Vivo.

First Author  Klochendler A Year  2016
Journal  Diabetes Volume  65
Issue  7 Pages  2081-93
PubMed ID  26993067 Mgi Jnum  J:249458
Mgi Id  MGI:5923592 Doi  10.2337/db16-0003
Citation  Klochendler A, et al. (2016) The Genetic Program of Pancreatic beta-Cell Replication In Vivo. Diabetes 65(7):2081-93
abstractText  The molecular program underlying infrequent replication of pancreatic beta-cells remains largely inaccessible. Using transgenic mice expressing green fluorescent protein in cycling cells, we sorted live, replicating beta-cells and determined their transcriptome. Replicating beta-cells upregulate hundreds of proliferation-related genes, along with many novel putative cell cycle components. Strikingly, genes involved in beta-cell functions, namely, glucose sensing and insulin secretion, were repressed. Further studies using single-molecule RNA in situ hybridization revealed that in fact, replicating beta-cells double the amount of RNA for most genes, but this upregulation excludes genes involved in beta-cell function. These data suggest that the quiescence-proliferation transition involves global amplification of gene expression, except for a subset of tissue-specific genes, which are "left behind" and whose relative mRNA amount decreases. Our work provides a unique resource for the study of replicating beta-cells in vivo.
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