Cell Reports (Feb 2021)

Inhibition of FGF10-ERK signal activation suppresses intraductal papillary neoplasm of the bile duct and its associated carcinomas

  • Hiroyuki Tomita,
  • Kaori Tanaka,
  • Akihiro Hirata,
  • Hideshi Okada,
  • Hisashi Imai,
  • Yohei Shirakami,
  • Kotaro Ohnishi,
  • Shigeyuki Sugie,
  • Hitomi Aoki,
  • Yuichiro Hatano,
  • Kei Noguchi,
  • Tomohiro Kanayama,
  • Ayumi Niwa,
  • Natsuko Suzui,
  • Tatsuhiko Miyazaki,
  • Takuji Tanaka,
  • Haruhiko Akiyama,
  • Masahito Shimizu,
  • Kazuhiro Yoshida,
  • Akira Hara

Journal volume & issue
Vol. 34, no. 8
p. 108772

Abstract

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Summary: Evidence regarding intraductal papillary neoplasm of the bile duct (IPNB) as a type of precancerous lesion of cholangiocarcinoma is limited. Moreover, a reproducible in vivo model is lacking, and IPNB pathogenesis remains unclear. Here, we use a doxycycline-inducible tetracycline (Tet)-on mice model to control fibroblast growth factor 10 (FGF10) expression, which regulates branching and tubule formation. FGF10-induced IPNB mimics the multifocal and divergent human IPNB phenotypes via the FGF10-FGF receptor 2 (FGFR2)-RAS-extracellular-signal-regulated kinase (ERK) signaling pathway. A paracrine/autocrine growth factor is sufficient to initiate and maintain IPNB originating from the peribiliary glands, including biliary stem/progenitor cells. With KrasG12D, p53, or p16 mutations or both, Fgf10-induced IPNB shows stepwise carcinogenesis, causing associated invasive carcinoma. Fgf10-induced papillary changes and progression are suppressed by the inhibition of the FGF10-FGFR2-RAS-ERK signaling pathway, demonstrating that the signal is a therapeutic target for IPNB and associated carcinoma.

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