AI Article Synopsis

  • Memory-phenotype (MP) CD4 T lymphocytes develop from naïve T cells and can differentiate into various T cell subsets to manage inflammation, especially in low-immune settings.
  • The study highlights that MP lymphocytes are not only made up of T helper 1 (T1) and T helper 17 (T17) cells but also contain a "undifferentiated" subpopulation that has the potential to develop into these functional subsets.
  • The undifferentiated MP lymphocytes possess the ability to proliferate rapidly and can differentiate into T1, T17, and regulatory T cells, which contributes to inflammation, although their response is regulated by existing T cells.

Article Abstract

Memory-phenotype (MP) CD4 T lymphocytes develop from naïve cells via self-recognition at homeostasis. While previous studies defined MP cells as a heterogeneous population that comprises T helper 1 (T1)/17-like subsets, functional significance of the T-bet Rorγt subpopulation remains unknown. Here we show that MP lymphocytes as a whole population can differentiate into T1/17/regulatory T (T) cells to mediate mild and persistent inflammation in lymphopenic environments, whereas naïve cells exhibit strong, T1-dominated responses. Moreover, we demonstrate that MP lymphocytes comprise not only T1/17-differentiated subsets but a polyclonal, transcriptomically immature "undifferentiated" subpopulation at homeostasis. Furthermore, our data argue that while the T-bet Rorγt MP subset is terminally T1-differentiated, its undifferentiated counterpart retains the capacity to rapidly proliferate to differentiate into T1/17/T cells, with the latter response tonically constrained by preexisting T cells. Together, our results identify undifferentiated MP CD4 T lymphocytes as a unique precursor that has a diverse differentiation potential to generate T1/17/T cells to contribute to pathogenesis of inflammation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11619248PMC
http://dx.doi.org/10.1126/sciadv.adq6618DOI Listing

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