Cholangiocytes with Mesenchymal Features Contribute to Progressive Hepatic Fibrosis of the Polycystic Kidney Rat

Yasunori Sato^*, Kenichi Harada^*, Satoru Ozaki^*, Shinichi Furubo, Kazuo Kizawa, Takahiro Sanzen, Mitsue Yasoshima^*, Hiroko Ikeda^*, Motoko Sasaki^* and Yasuni Nakanuma^*

From the Department of Human Pathology,^* Kanazawa University Graduate School of Medicine, Kanazawa; and the Drug Safety Research Laboratory, Toyama Chemical Company Limited, Toyama, Japan

The polycystic kidney (PCK) rat is an animal model of Caroli’sdisease with congenital hepatic fibrosis, in which the mechanismof progressive hepatic fibrosis remains unknown. This studyaimed to clarify the mechanism of hepatic fibrosis of the PCKrat from the viewpoint of the contribution of pathological cholangiocytes.In liver sections of the PCK rats, intrahepatic bile ducts wereconstituted by two different phenotypes: bile ducts lined bycuboidal-shaped and flat-shaped cholangiocytes. The flat-shapedcholangiocytes showed reduced immunohistochemical expressionof the biliary epithelial marker cytokeratin 19 and positiveimmunoreactivity for vimentin and fibronectin. When culturedcholangiocytes of the PCK rat were treated with transforminggrowth factor (TGF)-β1, a potent inducer of epithelial-mesenchymaltransition, induction of vimentin, fibronectin, and collagenexpression occurred in the PCK cholangiocytes. Although theTGF-β1 treatment reduced cytokeratin 19 expression, theepithelial cell features characterized by the expression ofE-cadherin and zonula occludens-1 was maintained, and ${alpha}$ -smoothmuscle actin expression was not induced in the cholangiocytes.Cholangiocytes of the PCK rat may acquire mesenchymal featuresin response to TGF-β1 and participate in progressive hepaticfibrosis by producing extracellular matrix molecules, whichseems to be a different event from epithelial-mesenchymal transition.