Cancer Medicine (Nov 2019)

Targeting claudin‐4 enhances chemosensitivity of pancreatic ductal carcinomas

  • Takamitsu Sasaki,
  • Rina Fujiwara‐Tani,
  • Shingo Kishi,
  • Shiori Mori,
  • Yi Luo,
  • Hitoshi Ohmori,
  • Isao Kawahara,
  • Kei Goto,
  • Yukiko Nishiguchi,
  • Takuya Mori,
  • Masayuki Sho,
  • Masuo Kondo,
  • Hiroki Kuniyasu

DOI
https://doi.org/10.1002/cam4.2547
Journal volume & issue
Vol. 8, no. 15
pp. 6700 – 6708

Abstract

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Abstract Claudin (CLDN) family comprises of protein that form a tight junction, and is involved in regulating polarity and differentiation of cells. Here, we aimed to investigate the effects of inhibiting CLDN4 in pancreatic ductal carcinomas (PDC). We first examined 91 cases of human PDC by immunohistochemistry and found that CLDN4 expression was correlated with tumor invasion, nodal metastasis, and distant metastasis. Anti‐CLDN4 extracellular domain antibody, previously established by us (4D3), inhibited the proliferation of MIA‐PaCa‐2 PDC cells and increased intracellular 5‐fluorouracil (5‐FU) concentration with lowering transepithelial electrical resistance. Concurrent treatment of 5‐FU and 4D3 resulted in synergistic inhibition of growth of MIA‐PaCa‐2 cells in nude mice. In addition, MIA‐PaCa‐2 cell tumors treated with full‐dose folfirinox (FFX) decreased tumor diameters to 50%; however, 60% of mice were dead from adverse effects. In contrast, half‐dose FFX concomitant with 4D3 treatment decreased tumors equivalent to full‐dose FFX, but without the adverse effects. These findings suggest that targeting CLDN4 might increase the effectiveness and safety of anticancer drug therapy in PDC.

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