Chd8 regulates X chromosome inactivation in mouse through fine-tuning control of Xist expression

Authors :: Nerea Blanes Ruiz
Giuseppe Trigiante
Monica Di Giacomo
Alexander N. Young
Gabrielle M Sant
Sarah J. Marzi
Andrea Cerase
Andreas Buness
Andreas Hierholzer
Philip Avner
Manish Kumar
Michela Ascolani
Mirjam Arnold
Source :: Communications Biology, Communications Biology, 4 (1), Communications Biology, Vol 4, Iss 1, Pp 1-13 (2021)
Publication Year :: 2021
Publisher :: Nature Publishing Group UK, 2021.
Abstract: Female mammals achieve dosage compensation by inactivating one of their two X chromosomes during development, a process entirely dependent on Xist, an X-linked long non-coding RNA (lncRNA). At the onset of X chromosome inactivation (XCI), Xist is up-regulated and spreads along the future inactive X chromosome. Contextually, it recruits repressive histone and DNA modifiers that transcriptionally silence the X chromosome. Xist regulation is tightly coupled to differentiation and its expression is under the control of both pluripotency and epigenetic factors. Recent evidence has suggested that chromatin remodelers accumulate at the X Inactivation Center (XIC) and here we demonstrate a new role for Chd8 in Xist regulation in differentiating ES cells, linked to its control and prevention of spurious transcription factor interactions occurring within Xist regulatory regions. Our findings have a broader relevance, in the context of complex, developmentally-regulated gene expression.<br />Communications Biology, 4 (1)<br />ISSN:2399-3642

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