Biomolecules (Jul 2021)

Neurotransmitter Profiles Are Altered in the Gut and Brain of Mice Mono-Associated with <i>Bifidobacterium dentium</i>

  • Berkley Luck,
  • Thomas D. Horvath,
  • Kristen A. Engevik,
  • Wenly Ruan,
  • Sigmund J. Haidacher,
  • Kathleen M. Hoch,
  • Numan Oezguen,
  • Jennifer K. Spinler,
  • Anthony M. Haag,
  • James Versalovic,
  • Melinda A. Engevik

DOI
https://doi.org/10.3390/biom11081091
Journal volume & issue
Vol. 11, no. 8
p. 1091

Abstract

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Background: Accumulating evidence indicates that the gut microbiota can synthesize neurotransmitters as well as impact host-derived neurotransmitter levels. In the past, it has been challenging to decipher which microbes influence neurotransmitters due to the complexity of the gut microbiota. Methods: To address whether a single microbe, Bifidobacterium dentium, could regulate important neurotransmitters, we examined Bifidobacteria genomes and explored neurotransmitter pathways in secreted cell-free supernatant using LC-MS/MS. To determine if B. dentium could impact neurotransmitters in vivo, we mono-associated germ-free mice with B. dentium ATCC 27678 and examined fecal and brain neurotransmitter concentrations. Results: We found that B. dentium possessed the enzymatic machinery to generate γ-aminobutyric acid (GABA) from glutamate, glutamine, and succinate. Consistent with the genome analysis, we found that B. dentium secreted GABA in a fully defined microbial media and elevated fecal GABA in B. dentium mono-associated mice compared to germ-free controls. We also examined the tyrosine/dopamine pathway and found that B. dentium could synthesize tyrosine, but could not generate L-dopa, dopamine, norepinephrine, or epinephrine. In vivo, we found that B. dentium mono-associated mice had elevated levels of tyrosine in the feces and brain. Conclusions: These data indicate that B. dentium can contribute to in vivo neurotransmitter regulation.

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