miR-302 regulates pancreatic progenitor pool and pancreatic size
Ziyue Z. Yang, Caroline G. Snider, Ronald J. Parchem

TL;DR
This study shows that miR-302 controls the number of pancreatic progenitor cells, which affects the size of the developing pancreas.
Contribution
The study provides the first comprehensive miRNA profile during early pancreatic development and identifies miR-302 as a key regulator.
Findings
miR-302 is highly enriched during early pancreatic development.
Loss of miR-302 reduces pancreatic size by decreasing progenitor cell proliferation.
miR-302 modulates genes related to Wnt signaling and cell cycle progression.
Abstract
Disruptions in pancreatic development can lead to health issues such as pancreatic agenesis and congenital diabetes mellitus. Understanding pancreatic organogenesis is critical for elucidating disease mechanisms and developing regenerative therapies. The pancreas consists of endocrine and exocrine cells, both of which are derived from multipotent progenitor cells (MPCs). MPC proliferation and differentiation are tightly controlled by multiple mechanisms, including post-transcriptional regulation by miRNAs. However, these regulatory factors are not fully understood. Here, we profiled miRNA expression in MPCs and identified that mir-302 was highly enriched during the earliest stages of pancreatic development. Loss of mir-302 resulted in reduced pancreatic size without altering the proportions of endocrine and exocrine cells at E17.5, suggesting that mir-302 regulates the number of MPCs…
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Taxonomy
TopicsPancreatic function and diabetes · Pancreatitis Pathology and Treatment · Congenital heart defects research
