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Phenotypic and in vivo functional characterization of immortalized human fetal liver cells.


ABSTRACT: We report the establishment and characterization of immortalized human fetal liver progenitor cells by expression of the Simian virus 40 large T (SV40 LT) antigen. Well-characterized cells at various passages were transplanted into nude mice with acute liver injury and tested for functional capacity. The SV40LT antigen-immortalized fetal liver cells showed a morphology similar to primary cells. Cultured cells demonstrated stable phenotypic expression in various passages, of hepatic markers such as albumin, CK 8, CK18, transcription factors HNF-4? and HNF-1? and CYP3A/7. The cells did not stain for any of the tested cancer-associated markers. Albumin, HNF-4? and CYP3A7 expression was confirmed by reverse transcription polymerase chain reaction (RT-PCR). Flow cytometry showed expression of some progenitor cell markers. In vivo study showed that the cells expressed both fetal and differentiated hepatocytes markers. Our study suggests new approaches to expand hepatic progenitor cells, analyze their fate in animal models aiming at cell therapy of hepatic diseases.

SUBMITTER: Patil PB 

PROVIDER: S-EPMC4059185 | biostudies-literature | 2014 Jun

REPOSITORIES: biostudies-literature

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Phenotypic and in vivo functional characterization of immortalized human fetal liver cells.

Patil Pradeep B PB   Begum Setara S   Joshi Meghnad M   Kleman Marika I MI   Olausson Michael M   Sumitran-Holgersson Suchitra S  

Scandinavian journal of gastroenterology 20140415 6


We report the establishment and characterization of immortalized human fetal liver progenitor cells by expression of the Simian virus 40 large T (SV40 LT) antigen. Well-characterized cells at various passages were transplanted into nude mice with acute liver injury and tested for functional capacity. The SV40LT antigen-immortalized fetal liver cells showed a morphology similar to primary cells. Cultured cells demonstrated stable phenotypic expression in various passages, of hepatic markers such  ...[more]

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