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Multiple inflammatory cytokine-productive ThyL-6 cell line established from a patient with thymic carcinoma

Authors :
Nobuo Takimoto
Sakon Noriki
Kunihiro Inai
Hiromi Okada
Yoshiaki Imamura
Hironobu Naiki
Takanori Ueda
Kazutaka Takagi
Source :
Cancer Science. 99:1778-1784
Publication Year :
2008
Publisher :
Wiley, 2008.

Abstract

Thymic epithelial cells can produce many kinds of cytokines, and interleukin (IL)-6-producing thymic carcinoma cases have been reported. However, a cytokine-producing human thymic tumor cell line has not previously been established. In this paper, we report a novel, multiple inflammatory cytokine-productive cell line that was established from a patient with thymic carcinoma. This cell line, designated ThyL-6, positively expressed epithelial membrane antigen, cytokeratins, vimentin intermediate filament and CD5, although hematological markers were not present in the cells. Cytokine antibody array analysis showed that the cells secreted several cytokines including IL-1alpha, IL-6, IL-8, RANTES, soluble TNFalpha-receptor 1, VEGF and CTLA into the culture medium. The addition of ThyL-6-cultured supernatant supported the growth of human myeloma ILKM-3 cells, which require the presence of IL-6 in the culture medium for the maintenance of cell growth, suggesting that the secreted IL-6 from ThyL-6 cells was biologically active. Chromosome analysis demonstrated that ThyL-6 cells had complex karyotype anomalies, including der(16)t(1;16); the latter has been recognized in thymic squamous cell carcinoma and thymic sarcomatoid carcinoma cases, as well as in several other kinds of malignancies. Heterotransplantation of the cells into nude mice showed tumorigenesis with neutrophil infiltration and liquefactive necrosis. These findings suggest that ThyL-6 cells will provide us with a new experimental tool for investigating not only the pathogenesis, biological behavior, chromo-somal analysis and therapeutic reagents of human thymic carcinoma, but also for studying cytokine-chemokine network systems.

Details

ISSN :
13497006 and 13479032
Volume :
99
Database :
OpenAIRE
Journal :
Cancer Science
Accession number :
edsair.doi.dedup.....be933c7d23314bbe1582429fca114c6f
Full Text :
https://doi.org/10.1111/j.1349-7006.2008.00897.x