AI Article Synopsis

  • Human microbiota begins forming at birth, influenced by maternal and environmental microbes, with core theories suggesting that initial colonizers impact community development.
  • Research involving 1,288 UK neonates revealed three distinct gut microbiota profiles, each led by specific microbial species affected by factors like maternal age and ethnicity.
  • Bifidobacteria, especially B. breve, were identified as key players in fostering stable gut microbiota and resisting pathogens, supporting their importance as primary colonizers in early life.

Article Abstract

Human microbiota assembly commences at birth, seeded by both maternal and environmental microorganisms. Ecological theory postulates that primary colonizers dictate microbial community assembly outcomes, yet such microbial priority effects in the human gut remain underexplored. Here using longitudinal faecal metagenomics, we characterized neonatal microbiota assembly for a cohort of 1,288 neonates from the UK. We show that the pioneering neonatal gut microbiota can be stratified into one of three distinct community states, each dominated by a single microbial species and influenced by clinical and host factors, such as maternal age, ethnicity and parity. A community state dominated by Enterococcus faecalis displayed stochastic microbiota assembly with persistent high pathogen loads into infancy. In contrast, community states dominated by Bifidobacterium, specifically B. longum and particularly B. breve, exhibited a stable assembly trajectory and long-term pathogen colonization resistance, probably due to strain-specific functional adaptions to a breast milk-rich neonatal diet. Consistent with our human cohort observation, B. breve demonstrated priority effects and conferred pathogen colonization resistance in a germ-free mouse model. Our findings solidify the crucial role of Bifidobacteria as primary colonizers in shaping the microbiota assembly and functions in early life.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11445081PMC
http://dx.doi.org/10.1038/s41564-024-01804-9DOI Listing

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