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Heterogeneity of the intrahepatic biliary epithelium.

机译:肝内胆管上皮的异质性。

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The objectives of this review are to outline the recent findings related to the morphological heterogeneity of the biliary epithelium and the heterogeneous pathophysiological responses of different sized bile ducts to liver gastrointestinal hormones and peptides and liver injury/toxins with changes in apoptotic, proliferative and secretory activities. The knowledge of biliary function is rapidly increasing because of the recognition that biliary epithelial cells (cholangiocytes) are the targets of human cholangiopathies, which are characterized by proliferation/damage of bile ducts within a small range of sizes. The unique anatomy, morphology, innervation and vascularization of the biliary epithelium are consistent with function of cholangiocytes within different regions of the biliary tree. The in vivo models [e.g., bile duct ligation (BDL), partial hepatectomy, feeding of bile acids, carbon tetrachloride (CCl4) or alpha-naphthylisothiocyanate (ANIT)] and the in vivo experimental tools [e.g., freshly isolated small and large cholangiocytes or intrahepatic bile duct units (IBDU) and primary cultures of small and large murine cholangiocytes] have allowed us to demonstrate the morphological and functional heterogeneity of the intrahepatic biliary epithelium. These models demonstrated the differential secretory activities and the heterogeneous apoptotic and proliferative responses of different sized ducts. Similar to animal models of cholangiocyte proliferation/injury restricted to specific sized ducts, in human liver diseases bile duct damage predominates specific sized bile ducts. Future studies related to the functional heterogeneity of the intrahepatic biliary epithelium may disclose new pathophysiological treatments for patients with cholangiopathies.
机译:这篇综述的目的是概述与胆汁上皮形态异质性以及不同大小的胆管对肝胃肠激素和肽以及肝损伤/毒素的凋亡,增殖和分泌活动的变化有关的异质病理生理反应的最新发现。 。由于人们认识到胆管上皮细胞(胆管细胞)是人胆管病的靶标,因此胆道功能的知识正在迅速增加,其特征是在小范围内胆管的增生/损伤。胆管上皮细胞的独特解剖结构,形态,神经支配和血管化与胆管树不同区域内的胆管细胞功能一致。体内模型[例如,胆管结扎(BDL),部分肝切除术,胆汁酸,四氯化碳(CCl4)或α-萘基异硫氰酸酯(ANIT)的进食]和体内实验工具[例如,新鲜分离的大小胆管细胞或肝内胆管单位(IBDU)和大小鼠的胆管细胞的原代培养]使我们能够证明肝内胆管上皮的形态和功能异质性。这些模型证明了不同大小的导管的差异性分泌活动以及异质性凋亡和增殖反应。与限于特定大小的导管的胆管细胞增殖/损伤的动物模型相似,在人类肝脏疾病中,胆管损伤占主导地位的是特定大小的胆管。未来有关肝内胆管上皮功能异质性的研究可能会揭示胆管病患者的新病理生理治疗方法。

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