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MicroRNAs in acute pancreatitis: From pathogenesis to novel diagnosis and therapy

Yi YangCollege of Medicine Southwest Jiaotong University Chengdu ChinaQilin HuangCollege of Medicine Southwest Jiaotong University Chengdu ChinaChen LuoDepartment of General Surgery & Pancreatic Injury and Repair Key Laboratory of Sichuan Province The General Hospital of Western Theater Command (Chengdu Military General Hospital) Chengdu ChinaYi WenDepartment of General Surgery & Pancreatic Injury and Repair Key Laboratory of Sichuan Province The General Hospital of Western Theater Command (Chengdu Military General Hospital) Chengdu ChinaRuohong LiuDepartment of General Surgery & Pancreatic Injury and Repair Key Laboratory of Sichuan Province The General Hospital of Western Theater Command (Chengdu Military General Hospital) Chengdu ChinaHongyu SunDepartment of General Surgery & Pancreatic Injury and Repair Key Laboratory of Sichuan Province The General Hospital of Western Theater Command (Chengdu Military General Hospital) Chengdu ChinaLijun TangCollege of Medicine Southwest Jiaotong University Chengdu China
2019en
ABI

Аннотация

Acute pancreatitis (AP) is an inflammatory disorder initiated by activation of pancreatic zymogens, leading to pancreatic injury and systemic inflammatory response. MicroRNAs (miRNAs) have emerged as important regulators of gene expression and key players in human physiological and pathological processes. Discoveries over the past decade have confirmed that altered expression of miRNAs is implicated in the pathogenesis of AP. Indeed, a number of miRNAs have been found to be dysregulated in various cell types involved in AP such as acinar cells, macrophages, and lymphocytes. These aberrant miRNAs can regulate acinar cell necrosis and apoptosis, local and systemic inflammatory response, thereby contributing to the initiation and progression of AP. Moreover, patients with AP possess unique miRNA signatures when compared with healthy individuals or those with other diseases. In view of their stability and easy detection, therefore, miRNAs have the potential to act as biomarkers for the diagnosis and assessment of patients with AP. In this review, we provide an overview of the novel cellular and molecular mechanisms underlying the roles of miRNAs during the disease processes of AP, as well as the potential diagnosis and therapeutic biomarkers of miRNAs in patients with AP.

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