TY - JOUR AU - Fan, Yajuan AU - Gao, Yuan AU - Ma, Qingyan AU - Yang, Zai AU - Zhao, Binbin AU - He, Xiaoyan AU - Yang, Jian AU - Yan, Bin AU - Gao, Fengjie AU - Qian, Li AU - Wang, Wei AU - Zhu, Feng AU - Ma, Xiancang PY - 2022 M3 - Original Research TI - Multi-Omics Analysis Reveals Aberrant Gut-Metabolome-Immune Network in Schizophrenia JO - Frontiers in Immunology UR - https://www.frontiersin.org/articles/10.3389/fimmu.2022.812293 VL - 13 SN - 1664-3224 N2 - Schizophrenia (SCZ) is associated with several immune dysfunctions, including elevated levels of pro-inflammatory cytokines. Microorganisms and their metabolites have been found to regulate the immune system, and that intestinal microbiota is significantly disturbed in schizophrenic patients. To systematically investigate aberrant gut-metabolome-immune network in schizophrenia, we performed an integrative analysis of intestinal microbiota, serum metabolome, and serum inflammatory cytokines in 63 SCZ patients and 57 healthy controls using a multi-omics strategy. Eighteen differentially abundant metabolite clusters were altered in patients displayed higher cytokine levels, with a significant increase in pro-inflammatory metabolites and a significant decrease in anti-inflammatory metabolites (such as oleic acid and linolenic acid). The bacterial co-abundance groups in the gut displayed more numerous and stronger correlations with circulating metabolites than with cytokines. By integrating these data, we identified that certain bacteria might affect inflammatory cytokines by modulating host metabolites, such as amino acids and fatty acids. A random forest model was constructed based on omics data, and seven serum metabolites significantly associated with cytokines and α-diversity of intestinal microbiota were able to accurately distinguish the cases from the controls with an area under the receiver operating characteristic curve of 0.99. Our results indicated aberrant gut-metabolome-immune network in SCZ and gut microbiota may influence immune responses by regulating host metabolic processes. These findings suggest a mechanism by which microbial-derived metabolites regulated inflammatory cytokines and insights into the diagnosis and treatment of mental disorders from the microbial-immune system in the future. ER -