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Reprogramming of Cancer Cells into Induced Pluripotent Stem Cells Questionedopen access

Authors
Bang, Jin SeokChoi, Na YoungLee, MinseongKo, KisungPark, Yo SephKo, Kinarm
Issue Date
Nov-2019
Publisher
KOREAN SOC STEM CELL RESEARCH
Keywords
Induced pluripotent stem cells; iPSC generation; RNA-sequencing analysis; Pluripotency; Cancer cell reprogramming
Citation
INTERNATIONAL JOURNAL OF STEM CELLS, v.12, no.3, pp 430 - 439
Pages
10
Journal Title
INTERNATIONAL JOURNAL OF STEM CELLS
Volume
12
Number
3
Start Page
430
End Page
439
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/38662
DOI
10.15283/ijsc19067
ISSN
2005-3606
2005-5447
Abstract
Background and Objectives: Several recent studies have claimed that cancer cells can be reprogrammed into induced pluripotent stem cells (iPSCs). However, in most cases, cancer cells seem to be resistant to cellular reprogramming. Furthermore, the underlying mechanisms of limited reprogramming in cancer cells are largely unknown. Here, we identified the candidate barrier genes and their target genes at the early stage of reprogramming for investigating cancer reprogramming. Methods: We tried induction of pluripotency in normal human fibroblasts (BJ) and both human benign (MCF10A) and malignant (MCF7) breast cancer cell lines using a classical retroviral reprogramming method. We conducted RNA-sequencing analysis to compare the transcriptome of the three cell lines at early stage of reprogramming. Results: We could generate iPSCs from BJ, whereas we were unable to obtain iPSCs from cancer cell lines. To address the underlying mechanism of limited reprogramming in cancer cells, we identified 29 the candidate barrier genes based on RNA-sequencing data. In addition, we found 40 their target genes using Cytoscape software. Conclusions: Our data suggest that these genes might one of the roadblock for cancer cell reprogramming. Furthermore, we provide new insights into application of iPSCs technology in cancer cell field for therapeutic purposes.
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