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Multiscale footprints reveal the organization of cis-regulatory elements

Author

Listed:
  • Yan Hu

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Max A. Horlbeck

    (Broad Institute of MIT and Harvard
    Harvard University
    Boston Children’s Hospital)

  • Ruochi Zhang

    (Broad Institute of MIT and Harvard
    Harvard University
    Broad Institute of MIT and Harvard)

  • Sai Ma

    (Broad Institute of MIT and Harvard
    Harvard University
    Icahn School of Medicine at Mount Sinai)

  • Rojesh Shrestha

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Vinay K. Kartha

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Fabiana M. Duarte

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Conrad Hock

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Rachel E. Savage

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Ajay Labade

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Heidi Kletzien

    (Harvard University
    Harvard Medical School)

  • Alia Meliki

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Andrew Castillo

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Neva C. Durand

    (Broad Institute of MIT and Harvard)

  • Eugenio Mattei

    (Broad Institute of MIT and Harvard)

  • Lauren J. Anderson

    (Broad Institute of MIT and Harvard)

  • Tristan Tay

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Andrew S. Earl

    (Broad Institute of MIT and Harvard
    Harvard University)

  • Noam Shoresh

    (Broad Institute of MIT and Harvard)

  • Charles B. Epstein

    (Broad Institute of MIT and Harvard)

  • Amy J. Wagers

    (Harvard University
    Harvard Medical School)

  • Jason D. Buenrostro

    (Broad Institute of MIT and Harvard
    Harvard University)

Abstract

Cis-regulatory elements (CREs) control gene expression and are dynamic in their structure and function, reflecting changes in the composition of diverse effector proteins over time1. However, methods for measuring the organization of effector proteins at CREs across the genome are limited, hampering efforts to connect CRE structure to their function in cell fate and disease. Here we developed PRINT, a computational method that identifies footprints of DNA–protein interactions from bulk and single-cell chromatin accessibility data across multiple scales of protein size. Using these multiscale footprints, we created the seq2PRINT framework, which uses deep learning to allow precise inference of transcription factor and nucleosome binding and interprets regulatory logic at CREs. Applying seq2PRINT to single-cell chromatin accessibility data from human bone marrow, we observe sequential establishment and widening of CREs centred on pioneer factors across haematopoiesis. We further discover age-associated alterations in the structure of CREs in murine haematopoietic stem cells, including widespread reduction of nucleosome footprints and gain of de novo identified Ets composite motifs. Collectively, we establish a method for obtaining rich insights into DNA-binding protein dynamics from chromatin accessibility data, and reveal the architecture of regulatory elements across differentiation and ageing.

Suggested Citation

  • Yan Hu & Max A. Horlbeck & Ruochi Zhang & Sai Ma & Rojesh Shrestha & Vinay K. Kartha & Fabiana M. Duarte & Conrad Hock & Rachel E. Savage & Ajay Labade & Heidi Kletzien & Alia Meliki & Andrew Castillo, 2025. "Multiscale footprints reveal the organization of cis-regulatory elements," Nature, Nature, vol. 638(8051), pages 779-786, February.
  • Handle: RePEc:nat:nature:v:638:y:2025:i:8051:d:10.1038_s41586-024-08443-4
    DOI: 10.1038/s41586-024-08443-4
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