Reg family proteins contribute to inflammation and pancreatic stellate cells activation in chronic pancreatitis

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作者
Wenting Chen
Mai Imasaka
Miyu Lee
Hirokazu Fukui
Hiroshi Nishiura
Masaki Ohmuraya
机构
[1] Hyogo Medical University,Department of Genetics
[2] Hyogo Medical University,Division of Gastroenterology and Hepatology, Department of Internal Medicine
[3] Hyogo Medical University,Division of Functional Pathology, Department of Pathology
[4] Osaka Medical and Pharmaceutical University,Clinical Training Center
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Chronic pancreatitis (CP) is a disease characterized by the inflammation and destruction of pancreatic tissue, leading to the replacement of functional tissue with fibrotic tissue. The regenerating gene (Reg) family proteins have recently been implicated in the repair and regeneration of inflamed pancreatic tissue, though the exact mechanisms of their involvement in the pathogenesis of CP are not yet fully understood. To investigate the role of Reg family proteins in CP, we generated global knockout mice (Reg−/−) for Reg1-3 (Reg1,2,3a,3b,3d,3g) genes using the CRISPR/Cas9 system. We then investigated the effect of Reg family protein deficiency in a genetic model of CP (X-SPINK1) mice by knocking out Reg1-3 genes. We examined pancreatic morphology, inflammatory cytokines expression, and activation of pancreatic stellate cells (PSCs) at different ages. Reg−/− mice showed no abnormalities in general growth and pancreas development. Deficiency of Reg1-3 in CP mice led to a reduction in pancreatic parenchymal loss, decreased deposition of collagen, and reduced expression of proinflammatory cytokines. Additionally, Reg proteins were found to stimulate PSCs activation. Overall, our study suggests that Reg1-3 deficiency can lead to the remission of CP and Reg family proteins could be a potential therapeutic target for the treatment of CP.
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