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RNA binding by Periphilin plays an essential role in initiating silencing by the HUSH complex. | LitMetric

RNA binding by Periphilin plays an essential role in initiating silencing by the HUSH complex.

Nucleic Acids Res

Cambridge Institute of Therapeutic Immunology & Infectious Disease (CITIID), Jeffrey Cheah Biomedical Centre, Department of Medicine, University of Cambridge, Cambridge, CB2 0AW, UK.

Published: December 2024

AI Article Synopsis

  • The human silencing hub (HUSH) complex is an epigenetic system that silences retroelements in the genome, primarily through components like TASOR, MPP8, and Periphilin, which work together to facilitate chromatin modification.
  • Periphilin is identified as the main RNA-binding component of the HUSH complex, and its N-terminal domain is crucial for both RNA binding and the overall function of HUSH.
  • The study demonstrates that Periphilin can exert HUSH-dependent silencing even when artificially tethered to a transcript that normally would not be silenced, highlighting its importance in the complex's mechanism of action.

Article Abstract

The human silencing hub (HUSH) complex is a transcription-dependent, epigenetic repressor complex that provides a genome-wide immunosurveillance system for the recognition and silencing of newly-integrated retroelements. The core HUSH complex of TASOR, MPP8 and Periphilin, represses these retroelements through SETDB1-mediated H3K9me3 deposition and MORC2-dependent chromatin compaction. HUSH-dependent silencing is RNA-mediated, yet no HUSH component contains a recognised RNA-binding domain. Here we used an unbiased approach to identify which HUSH component was able to bind RNA and determine whether RNA-binding was essential for HUSH function. We identify Periphilin as the major RNA-binding component of the HUSH complex and show that Periphilin's N-terminal domain is essential for both RNA binding and HUSH function. Periphilin binding to RNA was independent of its interaction with TASOR or MPP8, as its N-terminal domain was sufficient for RNA targeting. The artificial tethering of Periphilin to a HUSH-insensitive, nascent transcript, enabled the HUSH-dependent silencing of the transcript. This tethering of Periphilin allowed the RNA-binding region of Periphilin to be removed such that only its C-terminal domain was required for oligomerisation and interaction with TASOR. We therefore show that Periphilin is the predominant RNA-binding protein of the HUSH complex and this RNA-binding is essential for HUSH activity.

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Source
http://dx.doi.org/10.1093/nar/gkae1165DOI Listing

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