The significance of CDT1 expression in non-cancerous and cancerous liver in cases with hepatocellular carcinoma

We previously reported that chromatin licensing and DNA replication factor 1 (CDT1) expression was associated with the extent of proliferation of atypical hepatocytes and the time to postoperative recurrence in cases of hepatocellular carcinoma (HCC). This study aimed to clarify the clinical significance or pathogenesis of CDT1 expression in noncancerous and cancerous liver cases with HCC. We investigated the association between the expression of CDT1 in non-cancerous or cancerous liver tissues and long-term outcome, histologic findings or biochemical examination results in 62 cases. We also examined the dual localization between CDT1 and ki-67, FbxW7, P57kip2, P53 and cMyc by confocal laser scanning microscopy. CDT1 mRNA expression was significantly higher in cancerous liver than in non-cancerous liver (P<0.0001). High CDT1 mRNA expression reveals the strong degree of inflammatory cell infiltration in lobules, high levels of serum transaminase, to show hepatic spare decline and poor long-term prognosis. CDT1 mRNA was highly expressed in a group of poorly differentiated cancer cells. CDT1 co-localized with Ki-67, P57kip2, Fbwx7, P53 and c-Myc in the nucleus or cytoplasm of hepatocytes and cancer cells. We found that CDT1 mRNA expression could represent the degree of hepatic spare ability and the high carcinogenic state.