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Cell type signatures in cell-free DNA fragmentation profiles reveal disease biology

Author

Listed:
  • Kate E. Stanley

    (Laboratory for Cytogenetics and Genome Research, KU Leuven
    Karolinska Institute)

  • Tatjana Jatsenko

    (Laboratory for Cytogenetics and Genome Research, KU Leuven)

  • Stefania Tuveri

    (Laboratory for Cytogenetics and Genome Research, KU Leuven)

  • Dhanya Sudhakaran

    (Laboratory for Cytogenetics and Genome Research, KU Leuven)

  • Lore Lannoo

    (University Hospitals Leuven)

  • Kristel Calsteren

    (University Hospitals Leuven)

  • Marie Borre

    (Laboratory for Functional Epigenetics, KU Leuven)

  • Ilse Parijs

    (University Hospitals Leuven)

  • Leen Coillie

    (University Hospitals Leuven)

  • Kris Bogaert

    (University Hospitals Leuven)

  • Rodrigo Almeida Toledo

    (Vall d’Hebron Institute of Oncology)

  • Liesbeth Lenaerts

    (KU Leuven)

  • Sabine Tejpar

    (KU Leuven)

  • Kevin Punie

    (University Hospitals Leuven)

  • Laura Y. Rengifo

    (Laboratory of Genetics of Malignant Diseases, KU Leuven)

  • Peter Vandenberghe

    (Laboratory of Genetics of Malignant Diseases, KU Leuven
    University Hospitals Leuven)

  • Bernard Thienpont

    (Laboratory for Functional Epigenetics, KU Leuven)

  • Joris Robert Vermeesch

    (Laboratory for Cytogenetics and Genome Research, KU Leuven)

Abstract

Circulating cell-free DNA (cfDNA) fragments have characteristics that are specific to the cell types that release them. Current methods for cfDNA deconvolution typically use disease tailored marker selection in a limited number of bulk tissues or cell lines. Here, we utilize single cell transcriptome data as a comprehensive cellular reference set for disease-agnostic cfDNA cell-of-origin analysis. We correlate cfDNA-inferred nucleosome spacing with gene expression to rank the relative contribution of over 490 cell types to plasma cfDNA. In 744 healthy individuals and patients, we uncover cell type signatures in support of emerging disease paradigms in oncology and prenatal care. We train predictive models that can differentiate patients with colorectal cancer (84.7%), early-stage breast cancer (90.1%), multiple myeloma (AUC 95.0%), and preeclampsia (88.3%) from matched controls. Importantly, our approach performs well in ultra-low coverage cfDNA datasets and can be readily transferred to diverse clinical settings for the expansion of liquid biopsy.

Suggested Citation

  • Kate E. Stanley & Tatjana Jatsenko & Stefania Tuveri & Dhanya Sudhakaran & Lore Lannoo & Kristel Calsteren & Marie Borre & Ilse Parijs & Leen Coillie & Kris Bogaert & Rodrigo Almeida Toledo & Liesbeth, 2024. "Cell type signatures in cell-free DNA fragmentation profiles reveal disease biology," Nature Communications, Nature, vol. 15(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-46435-0
    DOI: 10.1038/s41467-024-46435-0
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