Omics Studies of the Murine Intestinal Ecosystem Exposed to Subchronic and Mild Social Defeat Stress

Overview

Journal J Proteome Res

Publisher American Chemical Society

Specialty Biochemistry

Date 2016 Aug 3

PMID 27482843

Citations 32

Authors

Ayako Aoki-Yoshida

Reiji Aoki

Naoko Moriya

Tatsuhiko Goto

Yoshifumi Kubota

Atsushi Toyoda

Yoshiharu Takayama

Chise Suzuki

Affiliations

Soon will be listed here.

Abstract

The microbiota-gut-brain axis plays an important role in the development of stress-induced mental disorders. We previously established the subchronic and mild social defeat stress (sCSDS) model, a murine experimental model of depression, and investigated the metabolomic profiles of plasma and liver. Here we used omics approaches to identify stress-induced changes in the gastrointestinal tract. Mice exposed to sCSDS for 10 days showed the following changes: (1) elevation of cholic acid and reduction of 5-aminovaleric acid among cecal metabolites; (2) downregulation of genes involved in the immune response in the terminal ileum; (3) a shift in the diversity of the microbiota in cecal contents and feces; and (4) fluctuations in the concentrations of cecal metabolites produced by gut microbiota reflected in plasma and hepatic metabolites. Operational taxonomic units within the family Lachnospiraceae showed an inverse correlation with certain metabolites. The social interaction score correlated with cecal metabolites, IgA, and cecal and fecal microbiota, suggesting that sCSDS suppressed the ileal immune response, altering the balance of microbiota, which together with host cells and host enzymes resulted in a pattern of accumulated metabolites in the intestinal ecosystem distinct from that of control mice.

Citing Articles

Effects of subchronic and mild social defeat stress on the intestinal microbiota and fecal bile acid composition in mice.

Yamagishi N, Kyoui D, Moriya N, Aoki-Yoshida A, Goto T, Toyoda A Biosci Microbiota Food Health. 2024; 43(3):260-266.

PMID: 38966043 PMC: 11220325. DOI: 10.12938/bmfh.2023-095.

The Gut Microbiota and Major Depressive Disorder: Current Understanding and Novel Therapeutic Strategies.

Bahmani M, Mehrtabar S, Jafarizadeh A, Zoghi S, Sadeghpour Heravi F, Abbasi A Curr Pharm Biotechnol. 2024; 25(16):2089-2107.

PMID: 38288791 DOI: 10.2174/0113892010281892240116081031.

Impacts of Subchronic and Mild Social Defeat Stress on Plasma Putrefactive Metabolites and Cardiovascular Structure in Male Mice.

Toyoda A, Kawakami K, Amano Y, Nishizawa H, Nakamura S, Kawase T Int J Mol Sci. 2023; 24(2).

PMID: 36674752 PMC: 9866670. DOI: 10.3390/ijms24021237.

The Role of the Microbiome-Brain-Gut Axis in the Pathogenesis of Depressive Disorder.

Mlynarska E, Gadzinowska J, Tokarek J, Forycka J, Szuman A, Franczyk B Nutrients. 2022; 14(9).

PMID: 35565888 PMC: 9105444. DOI: 10.3390/nu14091921.

Cross Brain-Gut Analysis Highlighted Hub Genes and LncRNA Networks Differentially Modified During Leucine Consumption and Endurance Exercise in Mice with Depression-Like Behaviors.

Abedpoor N, Taghian F, Hajibabaie F Mol Neurobiol. 2022; 59(7):4106-4123.

PMID: 35476290 PMC: 9045027. DOI: 10.1007/s12035-022-02835-1.