Chemical Impacts of the Microbiome Across Scales Reveal Novel Conjugated Bile Acids
Abstract
A mosaic of cross-phyla chemical interactions occurs between all metazoans and their microbiomes. In humans, the gut harbors the heaviest microbial load, but many organs, particularly those with a mucosal surface, associate with highly adapted and evolved microbial consortia. The microbial residents within these organ systems are increasingly well characterized, yielding a good understanding of human microbiome composition, but we have yet to elucidate the full chemical impact the microbiome exerts on an animal and the breadth of the chemical diversity it contributes. A number of molecular families are known to be shaped by the microbiome including short-chain fatty acids, indoles, aromatic amino acid metabolites, complex polysaccharides, and host lipids; such as sphingolipids and bile acids. These metabolites profoundly affect host physiology and are being explored for their roles in both health and disease. Considering the diversity of the human microbiome, numbering over 40,000 operational taxonomic units, a plethora of molecular diversity remains to be discovered. Here, we use unique mass spectrometry informatics approaches and data mapping onto a murine 3D-model to provide an untargeted assessment of the chemical diversity between germ-free (GF) and colonized mice (specific-pathogen free, SPF), and report the finding of novel bile acids produced by the microbiome in both mice and humans that have evaded characterization despite 170 years of research on bile acid chemistry.
Additional Information
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license. bioRxiv preprint first posted online Jun. 3, 2019. The authors would like to acknowledge funding from the National Institutes of Health under project 5U01AI124316-03, 1R03CA211211-01, 1R01HL116235 and R01HD084163. Additionally, B.S.B. was supported by UCSD KL2 (1KL2TR001444), J.L. by grant 13EIA14660045 from the American Heart Association. We would like to acknowledge Gail Ackerman for her contributions to curate the metadata. We further thank Alan Hofmann and Lee Hagey for their insightful discussions on structural characterization of bile acids. Data Availability: All metabolomics data is available at GNPS (g 232 nps.ucsd.edu) under the MassIVE id numbers: MSV000079949 (GF and SPF mouse data). Additional sample data: MSV000082480, MSV000082467, MSV000079134, MSV000082406. The sequencing data for the GF and SPF mouse study is available on the Qiita microbiome data analysis platform at Qiita.ucsd.edu under study ID 10801 and through the European Bioinformatics Institute accession number ERP109688. Author Contributions: PCD, RK and RQ designed the project. RQ, AA, AM, FV, JG, NG, AT, MC, ATN, MM, GH, RdS, and RB generated data. RQ, AV, AT and MC analyzed data. RQ, BB, ML, OP, JC, ML, JL, KP, BK, RJ, ME, KR, GH, KR, GC, WS and RB collected samples. PCD, RK, SM, VN and DS guided experimental 34 design and analysis. MW converted the data in GNPS, developed spectral search and molecular explorer. TT, VN and SM raised animals and guided experimental design. RQ and PD wrote the manuscript.Attached Files
Submitted - 654756v1.full.pdf
Supplemental Material - Figs_S1-S15.zip
Supplemental Material - media-16.docx
Supplemental Material - media-17.docx
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Additional details
- Alternative title
- Global Chemical Impacts of the Microbiome Include Unique Bile Acid Conjugates that Stimulate FXR
- Eprint ID
- 99619
- DOI
- 10.1101/654756
- Resolver ID
- CaltechAUTHORS:20191101-124547555
- 5U01AI124316-03
- NIH
- 1R03CA211211-01
- NIH
- 1R01HL116235
- NIH
- R01HD084163
- NIH
- 1KL2TR001444
- University of California, San Diego
- 13EIA14660045
- American Heart Association
- Created
-
2020-01-13Created from EPrint's datestamp field
- Updated
-
2021-11-16Created from EPrint's last_modified field
- Caltech groups
- Division of Biology and Biological Engineering