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   generation of an induced pluripotent stem cell line from human liver fibroblasts from a patient with combined hepatocellular-cholangiocarcinoma  
   
نویسنده ahn hyo-suk ,ryu jae-sung ,lee jaeseo ,mun seon ju ,hong yeon-hwa ,shin yongbo ,chung kyung-sook ,son myung jin
منبع cell journal (yakhteh) - 2022 - دوره : 24 - شماره : 3 - صفحه:133 -139
چکیده    Objective: combined hepatocellular-cholangiocarcinoma (chcc-cc) is a rare type of primary liver cancer with characteristics of both hepatocellular carcinoma (hcc) and cholangiocarcinoma (cc). the pathogenesis of chcccc is poorly understood due to a shortage of suitable in vitro models. due to scarce availability of human liver tissue, induced pluripotent stem cells (ipscs) are a useful alternative source to produce renewable liver cells. for use in the development of liver pathology models, here we successfully developed and evaluated ipscs from liver fibroblasts of a patient with chcc-cc. materials and methods: in this experimental study, human liver fibroblasts (hlfs) were obtained from the liver biopsy of a 69-year-old male patient with chcc-cc and transduced with a retroviral cocktail that included four factors - oct4, sox2, klf4, and c-myc (oskm). pluripotency of the ipscs was determined by alkaline phosphatase (ap) staining, quantitative real-time polymerase chain reaction (pcr), and immunofluorescence. we induced in vitro embryoid body (eb) formation and performed an in vivo teratoma assay to confirm their differentiation capacity into the three germ layers. results: hlf ipscs derived from the chcc-cc patient displayed typical ipsc-like morphology and pluripotency marker expression. the proficiency of the ipscs to differentiate into three germ layers was assessed both in vitro and in vivo. compared to normal control ipscs, differentiated hlf ipscs showed increased expressions of hcc markers alpha-fetoprotein (afp) and dickkopf-1 (dkk1) and the cc marker cytokeratin 7 (ck7), and a decreased expression of the cc tumour suppressor sry-related hmg-box 17 (sox17). conclusion: we established hlf ipscs using liver fibroblasts from a patient with chcc-cc for the first time. the hlf ipscs maintained marker expression in the patient when differentiated into ebs. therefore, hlf ipscs may be a sustainable cell source for modelling chcc-cc and beneficial for understanding liver cancer pathology and developing therapies for chcc-cc treatment.
کلیدواژه cholangiocarcinoma ,hepatocellular carcinoma ,induced pluripotent stem cells
آدرس korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea. korea university of science and technology (ust), department of functional genomics, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea. korea university of science and technology (ust), department of functional genomics, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea. korea university of science and technology (ust), department of functional genomics, south korea, korea university of science and technology (ust), department of functional genomics, south korea. korea research institute of bioscience and biotechnology (kribb), biomedical translational research center, south korea, korea research institute of bioscience and biotechnology (kribb), stem cell convergence research center, south korea. korea university of science and technology (ust), department of functional genomics, south korea
 
     
   
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