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Telomerase Reverse Transcriptase Related with Telomerase Activity Regulates Tumorigenic Potential of Mouse Embryonic Stem Cells

Authors
Park, Ki DaeSeong, Su KyoungPark, Yang MookChoi, YoungjuPark, Jae HyunLee, Sang-HunBaek, Dae HyunKang, Jin WookChoi, Kyoung SukPark, Sue NieKim, Dong SupKim, Seung HeeKim, Hyung Soo
Issue Date
Jan-2011
Publisher
MARY ANN LIEBERT, INC
Citation
STEM CELLS AND DEVELOPMENT, v.20, no.1, pp.149 - 157
Indexed
SCIE
SCOPUS
Journal Title
STEM CELLS AND DEVELOPMENT
Volume
20
Number
1
Start Page
149
End Page
157
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/169232
DOI
10.1089/scd.2009.0523
ISSN
1547-3287
Abstract
Embryonic stem cell (ESC) research gave rise to the possibility that stem cell therapy could be used in the treatment of incurable diseases such as neurodegenerative disorders. However, problems related to the tumorigenicity of undifferentiated ESCs must be resolved before such cells can be used in the application of cell replacement therapies. In the present study, we attempted to determine biomarkers that predicted tumor formation of undifferentiated ESCs in vivo. We differentiated mouse ESCs (R1 cell line) into neural lineage using a 5-step method, and evaluated the expression of oncogenes (p53, Bax, c-myc, Bcl2, K-ras), telomerase-related genes (TERT, TRF), and telomerase activity and telomere length during differentiation of ESCs. The expression of oncogenes did not show a significant change during differentiation steps, but the expression of telomerase reverse transcriptase (TERT) and telomerase activity correlated with mouse ESCs differentiation. To investigate the possibility of mouse TERT (mTERT) as a biomarker of tumorigenicity of undifferentiated ESCs, we established mTERT knockdown ESCs using the shRNA lentivirus vector and evaluated its tumorigenicity in vivo using nude mice. Tumor volumes significantly decreased, and appearances of tumor formation in mice were delayed in the TERT-knockdown ESC treated group compared with the undifferentiated ESC treated group. Altogether, these results suggested that mTERT might be potentially beneficial as a biomarker, rather than oncogenes of somatic cells, for the assessment of ESCs tumorigenicity.
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Lee, Sang Hun
COLLEGE OF MEDICINE (DEPARTMENT OF BIOCHEMISTRY & MOLECULAR BIOLOGY)
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