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Genome-wide analysis of PDX1 target genes in human pancreatic progenitors.


AUTHORS

Wang X , Sterr M , Burtscher I , Chen S , Hieronimus A , Machicao F , Staiger H , Häring HU , Lederer G , Meitinger T , Cernilogar FM , Schotta G , Irmler M , Beckers J , Hrabě de Angelis M , Ray M , Wright CVE , Bakhti M , Lickert H , . Molecular metabolism. 2018 1 30; ().

ABSTRACT

Homozygous loss-of-function mutations in the gene coding for the homeobox transcription factor (TF) PDX1 leads to pancreatic agenesis, whereas heterozygous mutations can cause Maturity-Onset Diabetes of the Young 4 (MODY4). Although the function of Pdx1 is well studied in pre-clinical models during insulin-producing β-cell development and homeostasis, it remains elusive how this TF controls human pancreas development by regulating a downstream transcriptional program. Also, comparative studies of PDX1 binding patterns in pancreatic progenitors and adult β-cells have not been conducted so far. Furthermore, many studies reported the association between single nucleotide polymorphisms (SNPs) and T2DM, and it has been shown that islet enhancers are enriched in T2DM-associated SNPs. Whether regions, harboring T2DM-associated SNPs are PDX1 bound and active at the pancreatic progenitor stage has not been reported so far.



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