@article{10.1172/jci.insight.141217, author = {Yun Weng AND Tyler J. Lieberthal AND Vivian X. Zhou AND Maya Lopez-Ichikawa AND Manuel Armas-Phan AND Tristan K. Bond AND Miya C. Yoshida AND Won-Tak Choi AND Tammy T. Chang}, journal = {JCI Insight}, publisher = {The American Society for Clinical Investigation}, title = {Liver epithelial focal adhesion kinase modulates fibrogenesis and hedgehog signaling}, year = {2020}, month = {10}, volume = {5}, url = {https://insight.jci.org/articles/view/141217}, abstract = {Focal adhesion kinase (FAK) is an important mediator of extracellular matrix–integrin mechano-signal transduction that regulates cell motility, survival, and proliferation. As such, FAK is being investigated as a potential therapeutic target for malignant and fibrotic diseases, and numerous clinical trials of FAK inhibitors are underway. The function of FAK in nonmalignant, nonmotile epithelial cells is not well understood. We previously showed that hepatocytes demonstrated activated FAK near stiff collagen tracts in fibrotic livers. In this study, we examined the role of liver epithelial FAK by inducing fibrotic liver disease in mice with liver epithelial FAK deficiency. We found that mice that lacked FAK in liver epithelial cells developed more severe liver injury and worse fibrosis as compared with controls. Increased fibrosis in liver epithelial FAK-deficient mice was linked to the activation of several profibrotic pathways, including the hedgehog/smoothened pathway. FAK-deficient hepatocytes produced increased Indian hedgehog in a manner dependent on matrix stiffness. Furthermore, expression of the hedgehog receptor, smoothened, was increased in macrophages and biliary cells of hepatocyte-specific FAK-deficient fibrotic livers. These results indicate that liver epithelial FAK has important regulatory roles in the response to liver injury and progression of fibrosis.}, number = {20}, doi = {10.1172/jci.insight.141217}, url = {https://doi.org/10.1172/jci.insight.141217}, }