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The transcription factor Duxbl mediates elimination of pre-T cells that fail β-selection.


ABSTRACT: T cell development is critically dependent on successful rearrangement of antigen-receptor chains. At the β-selection checkpoint, only cells with a functional rearrangement continue in development. However, how nonselected T cells proceed in their dead-end fate is not clear. We identified low CD27 expression to mark pre-T cells that have failed to rearrange their β-chain. Expression profiling and single-cell transcriptome clustering identified a developmental trajectory through β-selection and revealed specific expression of the transcription factor Duxbl at a stage of high recombination activity before β-selection. Conditional transgenic expression of Duxbl resulted in a developmental block at the DN3-to-DN4 transition due to reduced proliferation and enhanced apoptosis, whereas RNA silencing of Duxbl led to a decrease in apoptosis. Transcriptome analysis linked Duxbl to elevated expression of the apoptosis-inducing Oas/RNaseL pathway. RNaseL deficiency or sustained Bcl2 expression led to a partial rescue of cells in Duxbl transgenic mice. These findings identify Duxbl as a regulator of β-selection by inducing apoptosis in cells with a nonfunctional rearrangement.

SUBMITTER: Klein F 

PROVIDER: S-EPMC6400535 | biostudies-literature | 2019 Mar

REPOSITORIES: biostudies-literature

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The transcription factor Duxbl mediates elimination of pre-T cells that fail β-selection.

Klein Fabian F   Mitrovic Mladen M   Roux Julien J   Engdahl Corinne C   von Muenchow Lilly L   Alberti-Servera Llucia L   Fehling Hans Jörg HJ   Pelczar Pawel P   Rolink Antonius A   Tsapogas Panagiotis P  

The Journal of experimental medicine 20190214 3


T cell development is critically dependent on successful rearrangement of antigen-receptor chains. At the β-selection checkpoint, only cells with a functional rearrangement continue in development. However, how nonselected T cells proceed in their dead-end fate is not clear. We identified low CD27 expression to mark pre-T cells that have failed to rearrange their β-chain. Expression profiling and single-cell transcriptome clustering identified a developmental trajectory through β-selection and r  ...[more]

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