4.8 Article

Dedifferentiation process driven by TGF-beta signaling enhances stem cell properties in human colorectal cancer

期刊

ONCOGENE
卷 38, 期 6, 页码 780-793

出版社

NATURE PUBLISHING GROUP
DOI: 10.1038/s41388-018-0480-0

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资金

  1. JSPS [16H06391, 16H02662, 15K08970, 16H06250, 25860542, 15H04859]
  2. MEXT, Japan [25115002]
  3. Japan Agency for Medical Research and development, AMED [18cm0106507h0003, 18ck0106196h0003]
  4. Shinnihon Foundation of Advanced Medical Treatment Research
  5. AstraZeneca KK (AZKK Science Promotion Grant)
  6. Grants-in-Aid for Scientific Research [25860542, 16H06391, 16H06250, 15H04859, 16H02662, 15K08970] Funding Source: KAKEN

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Cancer stem cells (CSCs) possess the capacity for self-renewal and the potential to differentiate into non-CSCs. The recent discoveries of dynamic equilibrium between CSCs and non-CSCs revealed the significance of acquiring CSC-like properties in non-CSCs as an important process in progression of cancer. The mechanism underlying acquisition of CSC-like properties has mainly been investigated in the context of epithelial-mesenchymal transition. Here, we demonstrate the dedifferentiation process may be an alternative mechanism in acquisition of CSC-like properties in human colorectal cancer cells. By exploring the single-cell gene expression analysis of organoids developed from CD44(+) CSCs, we identified TWIST1 as a key molecule for maintaining the undifferentiated state of cancer cells. Consistent with the finding, we found that TGF-beta signaling pathway, a regulator of TWIST1, was specifically activated in the undifferentiated CD44(+) CSCs in human colorectal cancer using microarray-based gene expression analysis and quantitative pathology imaging system. Furthermore, we showed that external stimulation with TGF-beta and the induction of TWIST1 converted CD44(-) non-CSCs into the undifferentiated CD44(+) CSCs, leading to the significant increment of CSCs in xenograft models. This study strongly suggests dedifferentiation driven by TGF-beta signaling enhances stem cell properties in human colorectal cancer.

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