| Literature DB >> 31142539 |
Christian S M Helker1,2, Sri-Teja Mullapudi3, Laura M Mueller4, Jens Preussner5, Sorin Tunaru6,7, Oskar Skog8, Hyouk-Bum Kwon3, Florian Kreuder3, Joseph J Lancman9,10, Remy Bonnavion6, P Duc Si Dong9,10, Mario Looso5, Stefan Offermanns6, Ole Korsgren8, Francesca M Spagnoli4, Didier Y R Stainier1.
Abstract
An early step in pancreas development is marked by the expression of the transcription factor Pdx1 within the pancreatic endoderm, where it is required for the specification of all endocrine cell types. Subsequently, Pdx1 expression becomes restricted to the β-cell lineage, where it plays a central role in β-cell function. This pivotal role of Pdx1 at various stages of pancreas development makes it an attractive target to enhance pancreatic β-cell differentiation and increase β-cell function. In this study, we used a newly generated zebrafish reporter to screen over 8000 small molecules for modulators of pdx1 expression. We found four hit compounds and validated their efficacy at different stages of pancreas development. Notably, valproic acid treatment increased pancreatic endoderm formation, while inhibition of TGFβ signaling led to α-cell to β-cell transdifferentiation. HC toxin, another HDAC inhibitor, enhances β-cell function in primary mouse and human islets. Thus, using a whole organism screening strategy, this study identified new pdx1 expression modulators that can be used to influence different steps in pancreas and β-cell development.Entities:
Keywords: Pdx1; Small molecule screen; Transdifferentiation; α-Cells; β-Cells
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Year: 2019 PMID: 31142539 PMCID: PMC6679364 DOI: 10.1242/dev.172569
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868