4.8 Article

Rationally designed bacterial consortia to treat chronic immune-mediated colitis and restore intestinal homeostasis

Journal

NATURE COMMUNICATIONS
Volume 12, Issue 1, Pages -

Publisher

NATURE RESEARCH
DOI: 10.1038/s41467-021-23460-x

Keywords

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Funding

  1. Gusto Global LLC
  2. NIH [P40OD010995, P30DK034987, P01DK094779, R01ES024950, P30ES010126, R03ES032067, P42ES031007]
  3. Crohn's and Colitis Foundation

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Environmental factors, mucosal permeability, and defective immunoregulation contribute to overactive immunity towards certain intestinal bacteria, leading to various inflammatory conditions. GUT-108 expands beneficial gut bacteria, reduces pathogens, promotes mucosal healing and immune regulation.
Environmental factors, mucosal permeability and defective immunoregulation drive overactive immunity to a subset of resident intestinal bacteria that mediate multiple inflammatory conditions. GUT-103 and GUT-108, live biotherapeutic products rationally designed to complement missing or underrepresented functions in the dysbiotic microbiome of IBD patients, address upstream targets, rather than targeting a single cytokine to block downstream inflammation responses. GUT-103, composed of 17 strains that synergistically provide protective and sustained engraftment in the IBD inflammatory environment, prevented and treated chronic immune-mediated colitis. Therapeutic application of GUT-108 reversed established colitis in a humanized chronic T cell-mediated mouse model. It decreased pathobionts while expanding resident protective bacteria; produced metabolites promoting mucosal healing and immunoregulatory responses; decreased inflammatory cytokines and Th-1 and Th-17 cells; and induced interleukin-10-producing colonic regulatory cells, and IL-10-independent homeostatic pathways. We propose GUT-108 for treating and preventing relapse for IBD and other inflammatory conditions characterized by unbalanced microbiota and mucosal permeability.

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