Author:
Sen Akira,Imai Atsuki,Miyauchi Eiji,Yanagisawa Kota,Oda Tsukasa,Sasaki Fuki,Uchida Shintaro,Okada Takuhisa,Yokobori Takehiko,Saeki Hiroshi,Odamaki Toshitaka,Sasaki Nobuo
Abstract
AbstractThe large intestine has a dense milieu of indigenous bacteria, generating a complex ecosystem with crosstalk between individual bacteria and host cells.In vitrohost cell modeling and bacterial interactions at the anaerobic interphase have elucidated the crosstalk molecular basis. Although classical cell lines derived from patients with colorectal cancer including Caco-2 are used, whether they adequately mimic normal colonic epithelial physiology is unclear. To address this, we performed transcriptome profiling of Caco-2 and Monolayer-cultured epithelial cells derived from healthy Human Colonic Organoids (MHCO) cultured hemi-anaerobically. Coculture with the anaerobic gut bacteria,Bifidobacterium longumsubsp.longumdifferentiated the probiotic effects of test cells from those of physiologically normal intestinal and colorectal cancer cells. We cataloged non- or overlapping gene signatures where gene profiles of Caco-2 represented absorptive cells in the small intestinal epithelium, and MHCO showed complete colonic epithelium signature, including stem/progenitor, goblet, and enteroendocrine cells colonocytes. Characteristic gene expression changes related to lipid metabolism, inflammation, and cell-cell adhesion were observed in cocultured liveBifidobacterium longumand Caco-2 or MHCO.B. longum-stimulated MHCO exhibited barrier-enhancing characteristics, as demonstrated in clinical trials. Our data represent a valuable resource for understanding gut microbe and host cell communication.
Publisher
Cold Spring Harbor Laboratory