CTCF/RAD21 organize the ground state of chromatin-nuclear speckle association.

CTCF/RAD21 组织染色质-核斑点关联的基态

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作者:Yu Ruofan, Roseman Shelby, Siegenfeld Allison P, Gardner Zachary, Nguyen Son C, Tran Khoa A, Joyce Eric F, Jain Rajan, Liau Brian B, Krantz Ian D, Alexander Katherine A, Berger Shelley L
Recent findings indicate that nuclear speckles, a distinct type of nuclear body, interact with certain chromatin regions in a ground state. Here, we report that the chromatin structural factors CTCF and cohesin are required for full ground-state association between DNA and nuclear speckles. We identified a putative speckle-targeting motif (STM) within cohesin subunit RAD21 and demonstrated that the STM is required for chromatin-nuclear speckle association, disruption of which also impaired induction of speckle-associated genes. Depletion of the cohesin-releasing factor WAPL, which stabilizes cohesin on chromatin, resulted in reinforcement of DNA-speckle contacts and enhanced inducibility of speckle-associated genes. Additionally, we observed disruption of chromatin-nuclear speckle association in patient-derived cells with Cornelia de Lange syndrome, a congenital neurodevelopmental disorder involving defective cohesin pathways. In summary, our findings reveal a mechanism for establishing the ground state of chromatin-speckle association and promoting gene inducibility, with relevance to human disease.

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