A1 Vertaisarvioitu alkuperäisartikkeli tieteellisessä lehdessä

Maternal microbiota-derived metabolic profile in fetal murine intestine, brain and placenta




TekijätPessa-Morikawa Tiina, Husso Aleksi, Kärkkainen Olli, Koistinen Ville, Hanhineva Kati, Iivanainen Antti, Niku Mikael

KustantajaBMC

Julkaisuvuosi2022

JournalBMC Microbiology

Tietokannassa oleva lehden nimiBMC MICROBIOLOGY

Lehden akronyymiBMC MICROBIOL

Artikkelin numero 46

Vuosikerta22

Numero1

Sivujen määrä16

ISSN1471-2180

DOIhttps://doi.org/10.1186/s12866-022-02457-6

Verkko-osoitehttps://bmcmicrobiol.biomedcentral.com/articles/10.1186/s12866-022-02457-6

Rinnakkaistallenteen osoitehttps://research.utu.fi/converis/portal/detail/Publication/174899738


Tiivistelmä

Background

The maternal microbiota affects the development of the offspring by microbial metabolites translocating to the fetus. To reveal the spectrum of these molecular mediators of the earliest host-microbe interactions, we compared placenta, fetal intestine and brain from germ-free (GF) and specific pathogen free (SPF) mouse dams by non-targeted metabolic profiling.

Results

One hundred one annotated metabolites and altogether 3680 molecular features were present in significantly different amounts in the placenta and/or fetal organs of GF and SPF mice. More than half of these were more abundant in the SPF organs, suggesting their microbial origin or a metabolic response of the host to the presence of microbes. The clearest separation was observed in the placenta, but most of the molecular features showed significantly different levels also in the fetal intestine and/or brain. Metabolites that were detected in lower amounts in the GF fetal organs included 5-aminovaleric acid betaine, trimethylamine N-oxide, catechol-O-sulphate, hippuric and pipecolic acid. Derivatives of the amino acid tryptophan, such as kynurenine, 3-indolepropionic acid and hydroxyindoleacetic acid, were also less abundant in the absence of microbiota. Ninety-nine molecular features were detected only in the SPF mice. We also observed several molecular features which were more abundant in the GF mice, possibly representing precursors of microbial metabolites or indicators of a metabolic response to the absence of microbiota.

Conclusions

The maternal microbiota has a profound impact on the fetal metabolome. Our observations suggest the existence of a multitude of yet unidentified microbially modified metabolites which pass through the placenta into the fetus and potentially influence fetal development.


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