| Literature DB >> 32191873 |
Martin Trapecar1, Catherine Communal1, Jason Velazquez1, Christian Alexander Maass2, Yu-Ja Huang1, Kirsten Schneider1, Charles W Wright1, Vincent Butty3, George Eng4, Omer Yilmaz5, David Trumper6, Linda G Griffith7.
Abstract
Although the association between the microbiome and IBD and liver diseases is known, the cause and effect remain elusive. By connecting human microphysiological systems of the gut, liver, and circulating Treg and Th17 cells, we created a multi-organ model of ulcerative colitis (UC) ex vivo. The approach shows microbiome-derived short-chain fatty acids (SCFAs) to either improve or worsen UC severity, depending on the involvement of effector CD4 T cells. Using multiomics, we found SCFAs increased production of ketone bodies, glycolysis, and lipogenesis, while markedly reducing innate immune activation of the UC gut. However, during acute T cell-mediated inflammation, SCFAs exacerbated CD4+ T cell-effector function, partially through metabolic reprograming, leading to gut barrier disruption and hepatic injury. These paradoxical findings underscore the emerging utility of human physiomimetic technology in combination with systems immunology to study causality and the fundamental entanglement of immunity, metabolism, and tissue homeostasis.Entities:
Keywords: IBD; Th17; Treg; autoimmune hepatitis; gut-liver axis; immunometabolism; microphysiological system; physiomimetics; short-chain fatty acids; ulcerative colitis
Year: 2020 PMID: 32191873 PMCID: PMC8143761 DOI: 10.1016/j.cels.2020.02.008
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304