| Literature DB >> 28058178 |
Kohei Tatsumi1, Kazuo Ohashi1, Shigeki Mukobata1, Atsushi Kubo2, Fumikazu Koyama3, Yoshiyuki Nakajima3, Midori Shima4, Teruo Okano1.
Abstract
Coagulation factor IX (FIX) is synthesized by hepatocytes, and the lack of this protein causes hemophilia B. Liver nonparenchymal cells, including liver sinusoidal endothelial cells (LSECs) and extrahepatic cells in the body, are scarcely shown to have an ability to synthesize and secrete FIX. The present study investigated the existence of cells responsible for synthesizing FIX other than hepatocytes in mice using gene expression analyses and FIX-specific clotting assays. Among the several organs investigated, including liver, lung, spleen, kidney, brain, intestine, and tongue, FIX mRNA expressions were observed only in the liver. From the liver, hepatocytes and LSECs were isolated. FIX mRNA expression and FIX protein secretion were observed exclusively in the hepatocytes. Furthermore, the clotting activity of FIX secreted from the cultured hepatocytes was found to be dependent on the concentration of vitamin K2. These findings indicated that the hepatocyte is the only cell type that biochemically produces functional FIX in vivo. This highlights the importance of hepatocytes or cells that are fully differentiated toward the hepatic lineage for possible application for regenerative medicine and for targeting gene delivery to establish new cell-based treatments for hemophilia B.Entities:
Keywords: Factor IX; Hemophilia B; Hepatocyte; Nonparenchymal cell
Year: 2012 PMID: 28058178 PMCID: PMC5196924 DOI: 10.3727/215517912X639496
Source DB: PubMed Journal: Cell Med ISSN: 2155-1790