AI Article Synopsis

  • Certain guanine-rich sequences can form G-quadruplex (G4) structures, which are important for telomere protection and gene regulation but can hinder DNA replication if not resolved.
  • In the study, it was found that specific G4 sequences in the yeast Schizosaccharomyces pombe can form stable G4 structures, and the helicase Pfh1 can unwind them despite the presence of stabilizing compounds.
  • This research highlights the crucial function of G4 structures in ribosomal and telomeric DNA, underlining the conserved role of Pif1 helicases across different species in resolving these structures for genomic stability.

Article Abstract

Certain guanine-rich sequences have an inherent propensity to form G-quadruplex (G4) structures. G4 structures are e.g. involved in telomere protection and gene regulation. However, they also constitute obstacles during replication if they remain unresolved. To overcome these threats to genome integrity, organisms harbor specialized G4 unwinding helicases. In Schizosaccharomyces pombe, one such candidate helicase is Pfh1, an evolutionarily conserved Pif1 homolog. Here, we addressed whether putative G4 sequences in S. pombe can adopt G4 structures and, if so, whether Pfh1 can resolve them. We tested two G4 sequences, derived from S. pombe ribosomal and telomeric DNA regions, and demonstrated that they form inter- and intramolecular G4 structures, respectively. Also, Pfh1 was enriched in vivo at the ribosomal G4 DNA and telomeric sites. The nuclear isoform of Pfh1 (nPfh1) unwound both types of structure, and although the G4-stabilizing compound Phen-DC3 significantly enhanced their stability, nPfh1 still resolved them efficiently. However, stable G4 structures significantly inhibited adenosine triphosphate hydrolysis by nPfh1. Because ribosomal and telomeric DNA contain putative G4 regions conserved from yeasts to humans, our studies support the important role of G4 structure formation in these regions and provide further evidence for a conserved role for Pif1 helicases in resolving G4 structures.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5291255PMC
http://dx.doi.org/10.1093/nar/gkw349DOI Listing

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