Human gastric microbiota transplantation recapitulates premalignant lesions in germ-free mice

Author:

Kwon Soon-KyeongORCID,Park Jun ChulORCID,Kim Kwang HORCID,Yoon Jaekyung,Cho Yejin,Lee Buhyun,Lee Jin-Jae,Jeong Haengdueng,Oh Yeseul,Kim Sung-Hee,Lee So Dam,Hwang Bo Ram,Chung Yusook,Kim Jihyun FORCID,Nam Ki TaekORCID,Lee Yong ChanORCID

Abstract

ObjectiveGastric cancer (GC) is a leading cause of cancer-related mortality. Although microbes besides Helicobacter pylori may also contribute to gastric carcinogenesis, wild-type germ-free (GF) mouse models investigating the role of human gastric microbiota in the process are not yet available. We aimed to evaluate the histopathological features of GF mouse stomachs transplanted with gastric microbiota from patients with different gastric disease states and their relationships with the microbiota.DesignMicrobiota profiles in corpus and antrum tissues and gastric fluid from 12 patients with gastric dysplasia or GC were analysed. Thereafter, biopsied corpus and antrum tissues and gastric fluid from patients (n=15 and n=12, respectively) with chronic superficial gastritis, intestinal metaplasia or GC were inoculated into 42 GF C57BL/6 mice. The gastric microbiota was analysed by amplicon sequencing. Histopathological features of mouse stomachs were analysed immunohistochemically at 1 month after inoculation. An independent set of an additional 15 GF mice was also analysed at 1 year.ResultsThe microbial community structures of patients with dysplasia or GC in the corpus and antrum were similar. The gastric microbiota from patients with intestinal metaplasia or GC selectively colonised the mouse stomachs and induced premalignant lesions: loss of parietal cells and increases in inflammation foci, in F4/80 and Ki-67 expression, and in CD44v9/GSII lectin expression. Marked dysplastic changes were noted at 1 year post inoculation.ConclusionMajor histopathological features of premalignant changes are reproducible in GF mice transplanted with gastric microbiota from patients with intestinal metaplasia or GC. Our results suggest that GF mice are useful for analysing the causality of associations reported in human gastric microbiome studies.

Funder

Korea Health Technology R&D Project

Faculty Research Grant of Yonsei University College of Medicine

National Research Foundation of Korea

Publisher

BMJ

Subject

Gastroenterology

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