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Transcriptional responses of cancer cells to heat shock-inducing stimuli involve amplification of robust HSF1 binding

Author

Listed:
  • Sayantani Ghosh Dastidar

    (University of North Dakota School of Medicine
    Illumina, Inc.)

  • Bony Kumar

    (University of North Dakota School of Medicine
    Yale University School of Medicine)

  • Bo Lauckner

    (University of North Dakota School of Medicine)

  • Damien Parrello

    (University of North Dakota School of Medicine)

  • Danielle Perley

    (University of North Dakota School of Medicine
    McGill Genome Centre)

  • Maria Vlasenok

    (University of North Dakota School of Medicine
    Skolkovo Institute of Science and Technology)

  • Antariksh Tyagi

    (University of North Dakota School of Medicine
    Yale University School of Medicine)

  • Nii Koney-Kwaku Koney

    (University of North Dakota School of Medicine
    University of Ghana)

  • Ata Abbas

    (University of North Dakota School of Medicine
    Case Western Reserve University)

  • Sergei Nechaev

    (University of North Dakota School of Medicine)

Abstract

Responses of cells to stimuli are increasingly discovered to involve the binding of sequence-specific transcription factors outside of known target genes. We wanted to determine to what extent the genome-wide binding and function of a transcription factor are shaped by the cell type versus the stimulus. To do so, we induced the Heat Shock Response pathway in two different cancer cell lines with two different stimuli and related the binding of its master regulator HSF1 to nascent RNA and chromatin accessibility. Here, we show that HSF1 binding patterns retain their identity between basal conditions and under different magnitudes of activation, so that common HSF1 binding is globally associated with distinct transcription outcomes. HSF1-induced increase in DNA accessibility was modest in scale, but occurred predominantly at remote genomic sites. Apart from regulating transcription at existing elements including promoters and enhancers, HSF1 binding amplified during responses to stimuli may engage inactive chromatin.

Suggested Citation

  • Sayantani Ghosh Dastidar & Bony Kumar & Bo Lauckner & Damien Parrello & Danielle Perley & Maria Vlasenok & Antariksh Tyagi & Nii Koney-Kwaku Koney & Ata Abbas & Sergei Nechaev, 2023. "Transcriptional responses of cancer cells to heat shock-inducing stimuli involve amplification of robust HSF1 binding," Nature Communications, Nature, vol. 14(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-43157-7
    DOI: 10.1038/s41467-023-43157-7
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    References listed on IDEAS

    as
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