Tumor-associated MUC5AC stimulates in vivo tumorigenicity of human pancreatic cancer

  • Authors:
    • Hirotaka Hoshi
    • Tetsuji Sawada
    • Motoyuki Uchida
    • Hikaru Saito
    • Hiroko Iijima
    • Mikako Toda-Agetsuma
    • Tsutomu Wada
    • Sadaaki Yamazoe
    • Hiroaki Tanaka
    • Kenjiro Kimura
    • Anna Kakehashi
    • Min Wei
    • Kosei Hirakawa
    • Hideki Wanibuchi
  • View Affiliations

  • Published online on: January 18, 2011     https://doi.org/10.3892/ijo.2011.911
  • Pages: 619-627
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Abstract

MUC5AC, a high molecular weight glycoprotein, is overexpressed in the ductal region of human pancreatic cancer but is not detectable in the normal pancreas, suggesting its association with disease development. In the present study, we investigated the in vitro and in vivo effects of MUC5AC knockdown by short interfering RNA (siRNA) in the MUC5AC-overexpressing SW1990 and BxPC3 human pancreatic cancer cell lines in order to clarify its function. Significant decreases in the expression levels of MUC5AC mRNA and protein were observed in SW1990 and BxPC3 cells that had been stably transfected with a MUC5AC siRNA expression vector (SW1990/si-MUC5AC and BxPC3/si-MUC5AC cells) compared to those in cells transfected with an si-mock vector (SW1990/si-mock and BxPC3/si-mock cells). In in vitro studies, neither type of MUC5AC-knockdown cell showed any difference in cell survival, proliferation, or morphology from the si-mock cells or parental cells. However, in vivo xenograft studies demonstrated that MUC5AC knockdown significantly reduced the tumorigenicity and suppressed the tumor growth of si-MUC5AC cells compared to those of the si-mock cells. Immunohistochemical analysis revealed that CD45R/B220+ and Gr-1+ cells had infiltrated into the tumor tissue of the SW1990/si-MUC5AC cells. Furthermore, cancer-associated antigen specific antibodies were detected at high levels in the sera from the SW1990/si-MUC5AC cell-bearing mice. These results suggest that tumor-associated MUC5AC expressed on the surface of pancreatic cancer cells supports the escape of pancreatic cancer cells from immunosurveillance. The present findings highlight a new dimension of MUC5AC as a functional immunosuppressive agent and its important role in pancreatic cancer progression.

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March 2011
Volume 38 Issue 3

Print ISSN: 1019-6439
Online ISSN:1791-2423

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Spandidos Publications style
Hoshi H, Sawada T, Uchida M, Saito H, Iijima H, Toda-Agetsuma M, Wada T, Yamazoe S, Tanaka H, Kimura K, Kimura K, et al: Tumor-associated MUC5AC stimulates in vivo tumorigenicity of human pancreatic cancer. Int J Oncol 38: 619-627, 2011.
APA
Hoshi, H., Sawada, T., Uchida, M., Saito, H., Iijima, H., Toda-Agetsuma, M. ... Wanibuchi, H. (2011). Tumor-associated MUC5AC stimulates in vivo tumorigenicity of human pancreatic cancer. International Journal of Oncology, 38, 619-627. https://doi.org/10.3892/ijo.2011.911
MLA
Hoshi, H., Sawada, T., Uchida, M., Saito, H., Iijima, H., Toda-Agetsuma, M., Wada, T., Yamazoe, S., Tanaka, H., Kimura, K., Kakehashi, A., Wei, M., Hirakawa, K., Wanibuchi, H."Tumor-associated MUC5AC stimulates in vivo tumorigenicity of human pancreatic cancer". International Journal of Oncology 38.3 (2011): 619-627.
Chicago
Hoshi, H., Sawada, T., Uchida, M., Saito, H., Iijima, H., Toda-Agetsuma, M., Wada, T., Yamazoe, S., Tanaka, H., Kimura, K., Kakehashi, A., Wei, M., Hirakawa, K., Wanibuchi, H."Tumor-associated MUC5AC stimulates in vivo tumorigenicity of human pancreatic cancer". International Journal of Oncology 38, no. 3 (2011): 619-627. https://doi.org/10.3892/ijo.2011.911