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- HIF1-alpha Regulates Acinar Cell Function and Response to Injury in Mouse Pancreas.
HIF1-alpha Regulates Acinar Cell Function and Response to Injury in Mouse Pancreas.
Citation | “Hif1-Alpha Regulates Acinar Cell Function And Response To Injury In Mouse Pancreas.”. Gastroenterology, pp. 1630-1634.e3. . |
Center | University of Michigan |
Author | Min-Jung Park, Sapna Iyer, Xiang Xue, Juliana Bragazzi Cunha, Shufang Gu, David Moons, Steven W Pipe, John A Williams, Diane M Simeone, Yatrik M Shah, Bishr Omary |
Keywords | Blood Clotting, Factor VIII, Fibrinogen, Mouse Model |
Abstract |
We investigated whether intrapancreatic coagulation, with deposition of the fibrinogen-γ dimer (Fib-γD) and hypoxia, affect the severity of acute pancreatitis (AP) in mice. Pancreata of mice with AP induced by administration of cerulein or by L-arginine, or from patients with pancreatitis, had increased deposition of Fib-γD compared with control pancreata. Heparin administration protected mice from cerulein-induced AP and prevented Fib-γD formation. Cerulein administration resulted in activation and stabilization of hypoxia-inducible factor-1α (HIF1α) in pancreata of oxygen-dependent degradation domain-luciferase HIF1α reporter mice. Cerulein also led to induction of genes regulated by HIF1α, including Vegfa and Ero1a, before evidence of Fib-γD deposition or histologic features of AP. Expression of tissue factor, which is regulated by vascular endothelial growth factor, also increased following cerulein administration. Mice with acinar cell-specific disruption of Hif1a (Hif1a) developed spontaneous endoplasmic reticulum stress and less severe AP, but did not accumulate Fib-γD following administration of cerulein. Feeding mice increased pancreatic expression of HIF1α, indicating a physiologic role in the exocrine pancreas. Therefore, HIF1α has bifunctional roles, in exocrine pancreas homeostasis and progression of AP that is promoted by intrapancreatic coagulation. |
Year of Publication |
2018
|
Journal |
Gastroenterology
|
Volume |
154
|
Issue |
6
|
Number of Pages |
1630-1634.e3
|
Date Published |
12/2018
|
ISSN Number |
1528-0012
|
DOI |
10.1053/j.gastro.2018.01.037
|
Alternate Journal |
Gastroenterology
|
PMID |
29409830
|
PMCID |
PMC5927829
|
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