Human Smc5/6 recognises transcription-generated positive DNA supercoils.

Nat Commun

Department of Microbiology and Molecular Medicine, Faculty of Medicine, University of Geneva, Geneva 4, Switzerland.

Published: September 2024

AI Article Synopsis

  • The human Smc5/6 complex is crucial for chromosome stability and also functions as an antiviral factor by binding to and blocking transcription of extrachromosomal DNA.
  • It prefers to bind to circular DNA, and its recruitment is influenced by the transcription process, specifically the formation of DNA secondary structures.
  • Smc5/6 interacts with positively supercoiled DNA and is found at highly transcribed chromosome sites, revealing its role in managing DNA topology and highlighting how this contributes to antiviral defense.

Article Abstract

Beyond its essential roles in ensuring faithful chromosome segregation and genomic stability, the human Smc5/6 complex acts as an antiviral factor. It binds to and impedes the transcription of extrachromosomal DNA templates; an ability which is lost upon integration of the DNA into the chromosome. How the complex distinguishes among different DNA templates is unknown. Here we show that, in human cells, Smc5/6 preferentially binds to circular rather than linear extrachromosomal DNA. We further demonstrate that the transcriptional process, per se, and particularly the accumulation of DNA secondary structures known to be substrates for topoisomerases, is responsible for Smc5/6 recruitment. More specifically, we find that in vivo Smc5/6 binds to positively supercoiled DNA. Those findings, in conjunction with our genome-wide Smc5/6 binding analysis showing that Smc5/6 localizes at few but highly transcribed chromosome loci, not only unveil a previously unforeseen role of Smc5/6 in DNA topology management during transcription but highlight the significance of sensing DNA topology as an antiviral defense mechanism.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11379904PMC
http://dx.doi.org/10.1038/s41467-024-50646-wDOI Listing

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