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Single-cell transcriptomic and chromatin dynamics of the human brain in PTSD

Author

Listed:
  • Ahyeon Hwang

    (University of California Irvine
    University of California Irvine)

  • Mario Skarica

    (Yale University School of Medicine)

  • Siwei Xu

    (University of California Irvine)

  • Jensine Coudriet

    (Yale University School of Medicine)

  • Che Yu Lee

    (University of California Irvine)

  • Lin Lin

    (Yale University School of Medicine)

  • Rosemarie Terwilliger

    (Yale University School of Medicine)

  • Alexa-Nicole Sliby

    (Yale University School of Medicine)

  • Jiawei Wang

    (Yale University School of Medicine)

  • Tuan Nguyen

    (Yale University School of Medicine)

  • Hongyu Li

    (Yale University School of Medicine)

  • Min Wu

    (Yale University School of Medicine)

  • Yi Dai

    (University of California Irvine)

  • Ziheng Duan

    (University of California Irvine)

  • Shushrruth Sai Srinivasan

    (University of California Irvine
    University of California Irvine)

  • Xiangyu Zhang

    (Yale University School of Public Health)

  • Yingxin Lin

    (Yale University School of Public Health)

  • Dianne Cruz

    (Duke University Medical Center
    US Department of Veterans Affairs)

  • P. J. Michael Deans

    (Yale University School of Medicine)

  • Bertrand R. Huber

    (US Department of Veterans Affairs)

  • Daniel Levey

    (Yale University School of Medicine)

  • Jill R. Glausier

    (University of Pittsburgh School of Medicine)

  • David A. Lewis

    (University of Pittsburgh School of Medicine)

  • Joel Gelernter

    (Yale University School of Medicine
    US Department of Veterans Affairs)

  • Paul E. Holtzheimer

    (US Department of Veterans Affairs
    Geisel School of Medicine at Dartmouth)

  • Matthew J. Friedman

    (US Department of Veterans Affairs
    Geisel School of Medicine at Dartmouth)

  • Mark Gerstein

    (Yale University
    Yale University
    Yale University
    Yale University)

  • Nenad Sestan

    (Yale School of Medicine)

  • Kristen J. Brennand

    (Yale University School of Medicine
    Yale School of Medicine)

  • Ke Xu

    (Yale University School of Medicine
    US Department of Veterans Affairs)

  • Hongyu Zhao

    (Yale University School of Public Health)

  • John H. Krystal

    (Yale University School of Medicine
    US Department of Veterans Affairs)

  • Keith A. Young

    (Research Service
    Texas A&M University College of Medicine)

  • Douglas E. Williamson

    (Duke University Medical Center
    US Department of Veterans Affairs)

  • Alicia Che

    (Yale University School of Medicine)

  • Jing Zhang

    (University of California Irvine)

  • Matthew J. Girgenti

    (Yale University School of Medicine
    US Department of Veterans Affairs
    Yale School of Medicine)

Abstract

Post-traumatic stress disorder (PTSD) is a polygenic disorder occurring after extreme trauma exposure. Recent studies have begun to detail the molecular biology of PTSD. However, given the array of PTSD-perturbed molecular pathways identified so far1, it is implausible that a single cell type is responsible. Here we profile the molecular responses in over two million nuclei from the dorsolateral prefrontal cortex of 111 human brains, collected post-mortem from individuals with and without PTSD and major depressive disorder. We identify neuronal and non-neuronal cell-type clusters, gene expression changes and transcriptional regulators, and map the epigenomic regulome of PTSD in a cell-type-specific manner. Our analysis revealed PTSD-associated gene alterations in inhibitory neurons, endothelial cells and microglia and uncovered genes and pathways associated with glucocorticoid signalling, GABAergic transmission and neuroinflammation. We further validated these findings using cell-type-specific spatial transcriptomics, confirming disruption of key genes such as SST and FKBP5. By integrating genetic, transcriptomic and epigenetic data, we uncovered the regulatory mechanisms of credible variants that disrupt PTSD genes, including ELFN1, MAD1L1 and KCNIP4, in a cell-type-specific context. Together, these findings provide a comprehensive characterization of the cell-specific molecular regulatory mechanisms that underlie the persisting effects of traumatic stress response on the human prefrontal cortex.

Suggested Citation

  • Ahyeon Hwang & Mario Skarica & Siwei Xu & Jensine Coudriet & Che Yu Lee & Lin Lin & Rosemarie Terwilliger & Alexa-Nicole Sliby & Jiawei Wang & Tuan Nguyen & Hongyu Li & Min Wu & Yi Dai & Ziheng Duan &, 2025. "Single-cell transcriptomic and chromatin dynamics of the human brain in PTSD," Nature, Nature, vol. 643(8072), pages 744-754, July.
  • Handle: RePEc:nat:nature:v:643:y:2025:i:8072:d:10.1038_s41586-025-09083-y
    DOI: 10.1038/s41586-025-09083-y
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