Chinese Journal of Cancer Research

, Volume 17, Issue 1, pp 40–43 | Cite as

IFN-γ regulates Fas/FasL expression in cholangio carcinoma cells

Articles
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Abstracts

Objective: To study the regulation of Fas receptor (Fas)/Fas ligand (FasL) expression by IFN-γ in cholangiocarcinoma cell lines. Methods: We studied the expressions of Fas and FasL gene in the human cholangiocarcinoma cell line QBC939 by RT-PCR, Western blot, and immunohistochemistry and their apoptosis effects on human T cell line Jurkat cell. At the same time, we investigated the regulative effect of IFN-γ on them. Results: Fas, FasL mRNA and protein were expressed by cholangiocarcinoma cells. We also found IFN-γ could up-regulate the expressions of these two genes. However, IFN-γ could also down-regulate the ability of them to make Jurkat cells apoptotic. With the increasing of dosage and time, the effect was enhanced. Conclusion: IFN-γ could regulate the expression of Fas and FasL in cholangiocarcinoma cells, and might influence the ability of cholangiocarcinoma to regulate immune escape. This study provides new theoretical basis for immunological therapy of cholangiocarcinoma.

Key words

Cholangiocarcinoma Interferon Type II Apoptosis 

CLC number

R735.8 
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References

  1. [1]
    Jones BA, Gores GJ. Hepatobiliary malignancy [J]. Clin Liver Dis 1998; 2:437–49.PubMedCrossRefGoogle Scholar
  2. [2]
    O’Connell J, O’Sullivan GC, Collins JK, et al. The Fas counterattack: Fas-mediated T cell killing by colon cancer cells expressing Fas ligand [J]. J Exp Med 1996; 184:1075–82.PubMedCrossRefGoogle Scholar
  3. [3]
    Li DJ, Wang SG, Chen CH, et al. Effects of nm23-H1 gene transfection on proliferation of human QBC939 cholangiocarcinoma cell line [J]. Chin J Exp Srug 2004; 21:948–50.Google Scholar
  4. [4]
    Que FG, Phan VA, Phan VH, et al. Cholangiocarcinomas express Fas ligand and disable the Fas receptor [J]. Hepatology 1999; 30:1398–404.PubMedCrossRefGoogle Scholar
  5. [5]
    Shimonishi T, Isse K, Shibata F, et al. Up-regulation of fas ligand at early stages and down-regulation of Fas at progressed stages of intrahepatic cholangiocarcinoma reflect evasion from immune surveillance [J]. Hepatology 2000;32:761–9.PubMedCrossRefGoogle Scholar
  6. [6]
    von Bernstorff W, Spanjaard RA, Chan AK, et al. Pancreatic cancer cells can evade immune surveillance via nonfunctional Fas (APO-1/ CD95) receptors and aberrant expression of functional Fas ligand [J]. Surgery 1999; 125:73–84.CrossRefGoogle Scholar
  7. [7]
    von Reyher U, Strater J, Kittstein W, et al. Colon carcinoma cells use different mechanisms to escape CD95-mediated apoptosis [J]. Cancer Res 1998; 58:526–34.Google Scholar
  8. [8]
    Lebel M, Bertrand R, Mes-Masson AM. Decreased Fas antigen receptor expression in testicular tumor cell lines derived from polyomavirus large T-antigen transgenic mice [J]. Oncogene 1996; 12:1127–35.PubMedGoogle Scholar

Copyright information

© Chinese Journal 2005

Authors and Affiliations

  1. 1.Department of SurgeryPeking University School of Oncology, Beijing Institute for Cancer Research, Beijing Cancer HospitalBeijing

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