AI Article Synopsis

  • The thymus is responsible for producing T cells, with their development regulated by specific transcription factors and influenced by gut microbiota during early life.
  • Research shows that gut microbes affect the balance of certain T cell types in the thymus, highlighting the role of intestinal flora in immune system development.
  • Changes in thymic T cell populations due to early microbial exposure can have lasting impacts, potentially increasing vulnerability to immune-related diseases in adulthood.

Article Abstract

The thymus generates cells of the T cell lineage that seed the lymphatic and blood systems. Transcription factor regulatory networks control the lineage programming and maturation of thymic precursor cells. Whether extrathymic antigenic events, such as the microbial colonization of the mucosal tract also shape the thymic T cell repertoire is unclear. We show here that intestinal microbes influence the thymic homeostasis of PLZF-expressing cells in early life. Impaired thymic development of PLZF innate lymphocytes in germ-free (GF) neonatal mice is restored by colonization with a human commensal, , but not with a polysaccharide A (PSA) deficient isogenic strain. Plasmacytoid dendritic cells influenced by microbes migrate from the colon to the thymus in early life to regulate PLZF cell homeostasis. Importantly, perturbations in thymic PLZF cells brought about by alterations in early gut microbiota persist into adulthood and are associated with increased susceptibility to experimental colitis. Our studies identify a pathway of communication between intestinal microbes and thymic lymphocytes in the neonatal period that can modulate host susceptibility to immune-mediated diseases later in life.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7007548PMC
http://dx.doi.org/10.1073/pnas.1915047117DOI Listing

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