TABLE 1.
Notable examples of native or synthetic microbe consortia in therapy.
| Composition | Target disease/physiology | Mechanism of action | Model system | Ref |
|---|---|---|---|---|
| Selectively purified firmicutes spores from healthy human donors | CDI | Exact mechanism undefined. Possibly involves competitive exclusion of C. difficile presumably through secondary BA production (given the presence of firmicutes phyla) | Approved for human use (trade name VOWST) | Sims et al. (2023) |
| Microbiota suspension from healthy human donors | CDI | Competitive exclusion of C. difficile through an undefined mechanism | Approved for human use (trade name Rebyota) | Adolfsen et al. (2021) |
| Defined consortium of 33 gut commensals | CDI | Competitive exclusion of C. difficile through an unknown mechanism | Human clinical trial (NCT01372943) | Petrof et al. (2013) |
| Defined consortium of 11 gut commensals | Tumor, infection (immunomodulation) | Bacterial colonization, and bacterial antigen-mediated induction of interferon-γ-secretory CD8 T cells in colonic epithelial cells | Mouse | Tanoue et al. (2019) |
| C. scindens and engineered Bacteroides species (B. thetaiotaomicron, B. fragilis, or B. ovatus) | Immunomodulation | Induction of CD4+ regulatory T cells Treg cells | Mouse | Campbell et al. (2020) |
| Two step synthesis of 3β-hydroxydeoxycholic acid production from cholic acid via (i) cleavage of the 7α-hydroxyl group in cholic acid by Clostridium scindens, followed by (ii) epimerization of 3α-hydroxyl group in deoxycholic acid by engineered Bacteroides expressing hydroxysteroid dehydrogenases of Ruminococcus gnavus origin |