Thus, it seems reasonable to propose that the microenvironment (c

Thus, it seems reasonable to propose that the microenvironment (cirrhotic versus noncirrhotic) may be an important determinant of ICC histogenesis in these models. Of further interest, in both the Fan et al. and Sekiya and Suzuki studies, ICCs were observed to originate from transdifferentiated hepatocytes in the central areas of the liver lobule and not in the periportal areas, where the hepatic stem/progenitor cell niche is localized. However, the mechanisms underlying the centrilobular origin of transdifferented hepatocytes

and subsequent ICC development in these mouse models still need to be addressed. Although these findings are intriguing, it remains to be determined whether the development of ICCs from transdifferentiated hepatocytes has human clinical selleck chemicals relevance. Phenotypic biomarker studies performed as far back as the early 1980s have provided evidence of hepatocyte transdifferentiation into biliary epithelium in human livers under conditions of chronic hepatic injury and cholestasis,15 including established risk

conditions for ICC, such as primary sclerosing cholangitis, as well as plausible ICC risk conditions associated with chronic hepatic injury and inflammation selleck inhibitor (e.g., chronic hepatitis C infection, alchoholic hepatitis, and cirrhosis). However, it remains uncertain whether hepatocyte transdifferentiation to cholangiocytes plays a major role in ICC development

in patients with chronic hepatitis C (hepatitis C virus; HCV) or alcoholic liver disease. In this regard, it should be noted that BilIN, a recognized premalignant biliary lesion for human Org 27569 ICC in established risk conditions for ICC, has also been described in intrahepatic bile ducts of patients with chronic HCV and/or alcoholic-related cirrhosis.12, 13 Moreover, it is somewhat surprising that no HCC-CCA tumors were observed in livers of thioacetamide-treated mice genetically engineered to overexpress activated Notch in their hepatocytes, particularly because, in humans, this rare subtype is increasingly being reported in patients with chronic liver injury and cirrhosis.6, 18 Last, though it is currently appreciated that Notch signaling plays a critical role in biliary differentiation and morphogenesis, and is aberrantly overexpressed in human ICCs, Notch signaling has recently been reported to occur at a frequency of 30%-35% in analyzed cases of human HCCs, as well as to promote HCC development in genetically engineered mice.19 Interestingly, the HCCs that formed in these mice were mixed cell-type tumors containing both biliary and hepatocytic phenotypic features.

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