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Developmental And Cellular Age Direct Conversion Of Cd4(+) T Cells Into Ror Gamma(+) Or Helios(+) Colon Treg Cells

JOURNAL OF EXPERIMENTAL MEDICINE(2020)

Cited 49|Views19
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Abstract
ROR gamma(+) and Helios(+) Treg cells in the colon are phenotypically and functionally distinct, but their origins and relationships are poorly understood. In monocolonized and normal mice, single-cell RNA-seq revealed sharing of TCR clonotypes between these Treg cell populations, potentially denoting a common progenitor. In a polyclonal Treg cell replacement system, naive conventional CD4(+) (Tconv) cells, but not pre-existing tTregs, could differentiate into ROR gamma(+) pTregs upon interaction with gut microbiota. A smaller proportion of Tconv cells converted into Helios(+) pTreg cells, but these dominated when the Tconv cells originated from preweaning mice. T cells from infant mice were predominantly immature, insensitive to ROR gamma-inducing bacterial cues and to IL6, and showed evidence of higher TCR-transmitted signals, which are also characteristics of recent thymic emigrants (RTEs). Correspondingly, transfer of adult RTEs or Nur77(high) Tconv cells mainly yielded Helios(+) pTreg cells, recapitulating the infant/adult difference. Thus, CD4(+) Tconv cells can differentiate into both ROR gamma(+) and Helios(+) pTreg cells, providing a physiological adaptation of colonic Treg cells as a function of the age of the cell or of the individual.
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Key words
cellular age,cells
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