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  • Academic
    pdooley@stanford.edu
    University - Student Department: Department of Developmental Biology Position: Graduate

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All Publications

  • Thymic epithelial cells amplify epigenetic noise to promote immune tolerance. Nature Gamble, N., Caldwell, J. A., McKeever, J., Kaiser, C., Bradu, A., Dooley, P. J., Klemm, S., Greenleaf, W. J., Hibino, N., Dinner, A. R., Koh, A. S. 2025

    Abstract

    Cellular plasticity is a principal feature of vertebrate adaptation, tissue repair and tumorigenesis1,2. However, the mechanisms that regulate the stability of somatic cell fates remain unclear. Here, we use the somatic plasticity of thymic epithelial cells, which facilitates the selection of a self-discriminating T cell repertoire3, as a physiological model system to show that fluctuations in background chromatin accessibility in nucleosome-dense regions are amplified during thymic epithelial maturation for the ectopic expression of genes restricted to other specialized cell types. This chromatin destabilization was not dependent on AIRE-induced transcription but was preceded by repression of the tumour suppressor p53. Augmenting p53 activity indirectly stabilized chromatin, inhibited ectopic transcription, limited cellular plasticity and caused multi-organ autoimmunity. Genomic regions with heightened chromatin accessibility noise were selectively enriched for nucleosome-destabilizing polymeric AT tracts and were associated with elevated baseline DNA damage and transcriptional initiation. Taken together, our findings define molecular levers that modulateĀ cell fate integrity and areĀ used by thymic epithelial cells for immunological tolerance.

    View details for DOI 10.1038/s41586-025-09424-x

    View details for PubMedID 40836089

    View details for PubMedCentralID 5818993

https://orcid.org/0009-0008-0690-0313