Nature Communications (Mar 2025)

Endocrine-exocrine miR-503-322 drives aging-associated pancreatitis via targeting MKNK1 in acinar cells

  • Kerong Liu,
  • Tingting Lv,
  • Lu He,
  • Wei Tang,
  • Yan Zhang,
  • Xiao Xiao,
  • Yating Li,
  • Xiaoai Chang,
  • Shusen Wang,
  • Stephen J. Pandol,
  • Ling Li,
  • Xiao Han,
  • Yunxia Zhu

DOI
https://doi.org/10.1038/s41467-025-57615-x
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 16

Abstract

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Abstract Aging is the risk factor for chronic pancreatitis and severity determinant for its acute attack, yet the underlying cause is unclear. Here, we demonstrate that senescent β-cells of endocrine pancreas decide the onset and severity of chronic and acute pancreatitis. During physiological aging, senescent β-cells increase the expression of miR-503-322 which is secreted as small extracellular vesicles to enter exocrine acinar cells, driving a causal and reversible role on aging-associated pancreatitis. Mechanistically, miR-503-322 targets MKNK1 to inhibit acinar-cell secretion leading to autodigestion and repress proliferation causing repair damage of exocrine pancreas. In the elderly population, serum miR-503 concentration is negatively correlated with amylase, prone to chronic pancreatitis due to increased miR-503 and decreased MKNK1 in the elderly pancreas. Our findings highlight the miR-503-322–MKNK1 axis mediating the endocrine-exocrine regulatory pathway specifically in aged mice and humans. Modulating this axis may provide potential preventive and therapeutic strategies for aging-associated pancreatitis.