Microbial bile salt hydrolase activity influences gene expression profiles and gastrointestinal maturation in infant mice.
María A Núñez-SánchezFlorence M HerissonJonathan M KeaneNatalia García-GonzálezValerio RossiniJorge PinhieroJack DalyMilán Bustamante-GarridoCara M HuestonShriram PatelNuria CanelaPol HerreroMarcus J ClaessonSilvia MelgarKen NallyNoel M CapliceCormac G M GahanPublished in: Gut microbes (2022)
The mechanisms by which early microbial colonizers of the neonate influence gut development are poorly understood. Bacterial bile salt hydrolase (BSH) acts as a putative colonization factor that influences bile acid signatures and microbe-host signaling pathways and we considered whether this activity can influence infant gut development. In silico analysis of the human neonatal gut metagenome confirmed that BSH enzyme sequences are present as early as one day postpartum. Gastrointestinal delivery of cloned BSH to immature gnotobiotic mice accelerated shortening of the colon and regularized gene expression profiles, with monocolonised mice more closely resembling conventionally raised animals. In situ expression of BSH decreased markers of cell proliferation (Ki67, Hes2 and Ascl2) and strongly increased expression of ALPI, a marker of cell differentiation and barrier function. These data suggest an evolutionary paradigm whereby microbial BSH activity potentially influences bacterial colonization and in-turn benefits host gastrointestinal maturation.
Keyphrases
- gene expression
- microbial community
- high fat diet induced
- cell proliferation
- poor prognosis
- genome wide
- endothelial cells
- dna methylation
- binding protein
- pi k akt
- molecular docking
- squamous cell carcinoma
- insulin resistance
- copy number
- electronic health record
- radiation therapy
- epithelial mesenchymal transition
- lymph node
- adipose tissue
- genome wide analysis
- locally advanced