| Literature DB >> 31607563 |
Ruth A Singer1, Luis Arnes2, Yi Cui3, Jiguang Wang4, Yuqian Gao3, Michelle A Guney5, Kristin E Burnum-Johnson3, Raul Rabadan4, Charles Ansong3, Galya Orr3, Lori Sussel6.
Abstract
Many studies have highlighted the role of dysregulated glucagon secretion in the etiology of hyperglycemia and diabetes. Accordingly, understanding the mechanisms underlying pancreatic islet α cell development and function has important implications for the discovery of new therapies for diabetes. In this study, comparative transcriptome analyses between embryonic mouse pancreas and adult mouse islets identified several pancreatic lncRNAs that lie in close proximity to essential pancreatic transcription factors, including the Pax6-associated lncRNA Paupar. We demonstrate that Paupar is enriched in glucagon-producing α cells where it promotes the alternative splicing of Pax6 to an isoform required for activation of essential α cell genes. Consistently, deletion of Paupar in mice resulted in dysregulation of PAX6 α cell target genes and corresponding α cell dysfunction, including blunted glucagon secretion. These findings illustrate a distinct mechanism by which a pancreatic lncRNA can coordinate glucose homeostasis by cell-specific regulation of a broadly expressed transcription factor.Entities:
Keywords: Paupar; Pax6; diabetes; glucagon; lncRNAs; long noncoding RNAs; pancreatic islets; transcription factors; α cells
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Year: 2019 PMID: 31607563 PMCID: PMC7205457 DOI: 10.1016/j.cmet.2019.09.013
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287