Cellular and Molecular Gastroenterology and Hepatology (Jan 2019)

Generation of Human iPSC–Derived Intestinal Epithelial Cell Monolayers by CDX2 TransductionSummary

  • Kazuo Takayama,
  • Ryosuke Negoro,
  • Tomoki Yamashita,
  • Kanae Kawai,
  • Moe Ichikawa,
  • Takanori Mori,
  • Noriyuki Nakatsu,
  • Kazuo Harada,
  • Sumito Ito,
  • Hiroshi Yamada,
  • Yoshiyuki Yamaura,
  • Kazumasa Hirata,
  • Seiichi Ishida,
  • Hiroyuki Mizuguchi

Journal volume & issue
Vol. 8, no. 3
pp. 513 – 526

Abstract

Read online

Background & aims: To develop an effective and safe orally administered drug, it is important to predict its intestinal absorption rate, intestinal first-pass effect, and drug-drug interactions of orally administered drugs. However, there is no existing model to comprehensively predict the intestinal pharmacokinetics and drug-response of orally administered drugs. In this study, we attempted to generate homogenous and functional intestinal epithelial cells from human induced pluripotent stem (iPS) cells for pharmaceutical research. Methods: We generated almost-homogenous Villin- and zonula occludens-1 (ZO1)-positive intestinal epithelial cells by caudal-related homeobox transcription factor 2 (CDX2) transduction into human iPS cell-derived intestinal progenitor cells. Results: The drug absorption rates in human iPS cell-derived intestinal epithelial cell monolayers (iPS-IECM) were highly correlated with those in humans (R2=0.91). The expression levels of cytochrome P450 (CYP) 3A4, a dominant drug-metabolizing enzyme in the small intestine, in human iPS-IECM were similar to those in human small intestine in vivo. In addition, intestinal availability in human iPS-IECM (the fraction passing the gut wall: Fg=0.73) was more similar to that in the human small intestine in vivo (Fg=0.57) than to that in Caco-2 cells (Fg=0.99), a human colorectal adenocarcinoma cell line. Moreover, the drug-drug interaction and drug-food interaction could be observed by using our human iPS-IECM in the presence of an inducer and inhibitor of CYP3A4, i.e., rifampicin and grape fruit juice, respectively. Conclusion: Taking these results together, we succeeded in generating the human iPS-IECM that can be applied to various intestinal pharmacokinetics and drug-response tests of orally administered drugs. Keywords: CYP3A4, Intestinal First-Pass Effect, Differentiation, Adenovirus