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Dynamics of chromatin accessibility and long-range interactions in response to glucocorticoid pulsing.

Genome research (2015-02-14)
Diana A Stavreva, Antoine Coulon, Songjoon Baek, Myong-Hee Sung, Sam John, Lenka Stixova, Martina Tesikova, Ofir Hakim, Tina Miranda, Mary Hawkins, John A Stamatoyannopoulos, Carson C Chow, Gordon L Hager
RÉSUMÉ

Although physiological steroid levels are often pulsatile (ultradian), the genomic effects of this pulsatility are poorly understood. By utilizing glucocorticoid receptor (GR) signaling as a model system, we uncovered striking spatiotemporal relationships between receptor loading, lifetimes of the DNase I hypersensitivity sites (DHSs), long-range interactions, and gene regulation. We found that hormone-induced DHSs were enriched within ± 50 kb of GR-responsive genes and displayed a broad spectrum of lifetimes upon hormone withdrawal. These lifetimes dictate the strength of the DHS interactions with gene targets and contribute to gene regulation from a distance. Our results demonstrate that pulsatile and constant hormone stimulations induce unique, treatment-specific patterns of gene and regulatory element activation. These modes of activation have implications for corticosteroid function in vivo and for steroid therapies in various clinical settings.

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