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AIRE relies on Z-DNA to flag gene targets for thymic T cell tolerization

Author

Listed:
  • Yuan Fang

    (Harvard Medical School
    Harvard University)

  • Kushagra Bansal

    (Jawaharlal Nehru Centre for Advanced Scientific Research)

  • Sara Mostafavi

    (University of Washington
    Canadian Institute for Advanced Research)

  • Christophe Benoist

    (Harvard Medical School)

  • Diane Mathis

    (Harvard Medical School)

Abstract

AIRE is an unconventional transcription factor that enhances the expression of thousands of genes in medullary thymic epithelial cells and promotes clonal deletion or phenotypic diversion of self-reactive T cells1–4. The biological logic of AIRE’s target specificity remains largely unclear as, in contrast to many transcription factors, it does not bind to a particular DNA sequence motif. Here we implemented two orthogonal approaches to investigate AIRE’s cis-regulatory mechanisms: construction of a convolutional neural network and leveraging natural genetic variation through analysis of F1 hybrid mice5. Both approaches nominated Z-DNA and NFE2–MAF as putative positive influences on AIRE’s target choices. Genome-wide mapping studies revealed that Z-DNA-forming and NFE2L2-binding motifs were positively associated with the inherent ability of a gene’s promoter to generate DNA double-stranded breaks, and promoters showing strong double-stranded break generation were more likely to enter a poised state with accessible chromatin and already-assembled transcriptional machinery. Consequently, AIRE preferentially targets genes with poised promoters. We propose a model in which Z-DNA anchors the AIRE-mediated transcriptional program by enhancing double-stranded break generation and promoter poising. Beyond resolving a long-standing mechanistic conundrum, these findings suggest routes for manipulating T cell tolerance.

Suggested Citation

  • Yuan Fang & Kushagra Bansal & Sara Mostafavi & Christophe Benoist & Diane Mathis, 2024. "AIRE relies on Z-DNA to flag gene targets for thymic T cell tolerization," Nature, Nature, vol. 628(8007), pages 400-407, April.
  • Handle: RePEc:nat:nature:v:628:y:2024:i:8007:d:10.1038_s41586-024-07169-7
    DOI: 10.1038/s41586-024-07169-7
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