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Cited 10 time in webofscience Cited 8 time in scopus
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Establishment of Hepatocellular Cancer Induced Pluripotent Stem Cells Using a Reprogramming Techniqueopen access

Authors
Kim, Han JoonJeong, JaeminPark, SunhooJin, Young-WooLee, Seung-SookLee, Seung BumChoi, Dongho
Issue Date
Mar-2017
Publisher
EDITORIAL OFFICE GUT & LIVER
Keywords
Liver neoplasms; Induced pluripotent stem cells; Reprogramming
Citation
GUT AND LIVER, v.11, no.2, pp.261 - 269
Indexed
SCIE
SCOPUS
KCI
Journal Title
GUT AND LIVER
Volume
11
Number
2
Start Page
261
End Page
269
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/2477
DOI
10.5009/gnl15389
ISSN
1976-2283
Abstract
Background/Aims: Cancer is known to be a disease by many factors. However, specific results of reprogramming by pluripotency-related transcription factors remain to be scarcely reported. Here, we verified potential effects of pluripotent-related genes in hepatocellular carcinoma cancer cells. Methods: To better understand reprogramming of cancer cells in different genetic backgrounds, we used four liver cancer cell lines representing different states of p53 (HepG2, Hep3B, Huh7 and PLC). Retroviral-mediated introduction of reprogramming related genes (KLF4, Oct4, Sox2, and Myc) was used to induce the expression of proteins related to a pluripotent status in liver cancer cells. Results: Hep3B cells (null p53) exhibited a higher efficiency of reprogramming in comparison to the other liver cancer cell lines. The reprogrammed Hep3B cells acquired similar characteristics to pluripotent stem cells. However, loss of sternness in Hep3B-iPCs was detected during continual passage. Conclusions: We demonstrated that reprogramming was achieved in tumor cells through retroviral induction of genes associated with reprogramming. Interestingly, the reprogrammed pluripotent cancer cells (iPCs) were very different from original cancer cells in terms of colony shape and expressed markers. The induction of pluripotency of liver cancer cells correlated with the status of p53, suggesting that different expression level of p53 in cancer cells may affect their reprogramming.
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