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Potential in a single cancer cell to produce heterogeneous morphology, radiosensitivity and gene expression
Authors:Ban Sadayuki  Ishikawa Ken-Ichi  Kawai Seiko  Koyama-Saegusa Kumiko  Ishikawa Atsuko  Shimada Yutaka  Inazawa Johji  Imai Takashi
Affiliation:RadGenomics Project, Frontier Research Center, National Institute of Radiological Sciences, Anagawa, Chiba, Japan. s_ban@nirs.go.jp
Abstract:Morphologically heterogeneous colonies were formed from a cultured cell line (KYSE70) established from one human esophageal carcinoma tissue. Two subclones were separated from a single clone (clone13) of KYSE70 cells. One subclone (clone13-3G) formed mainly mounding colonies and the other (clone 13-6G) formed flat, diffusive colonies. X-irradiation stimulated the cells to dedifferentiate from the mounding state to the flat, diffusive state. Clone 13-6G cells were more radiosensitive than the other 3 cell lines. Clustering analysis for gene expression level by oligonucleotide microarray demonstrated that in the radiosensitive clone13-6G cells, expression of genes involved in cell adhesion was upregulated, but genes involved in the response to DNA damage stimulus were downregulated. The data demonstrated that a single cancer cell had the potential to produce progeny heterogeneous in terms of morphology, radiation sensitivity and gene expression, and irradiation enhanced the dedifferentiation of cancer cells.
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