4.8 Article

Short loop length and high thermal stability determine genomic instability induced by G-quadruplex-forming minisatellites

Journal

EMBO JOURNAL
Volume 34, Issue 12, Pages 1718-1734

Publisher

WILEY
DOI: 10.15252/embj.201490702

Keywords

genomic instability; G-quadruplex; minisatellite; Phen-DC3; Pif1

Funding

  1. Ministere de l'Education Nationale, de la Recherche, et de la Technologie (MENRT)
  2. Association pour la Recherche sur le Cancer (ARC)
  3. Fondation pour la Recherche Medicale (FRM)
  4. Yousef Jameel scholarship
  5. Singapore Ministry of Education Academic Research Fund Tier 3 [MOE2012-T3-1-001]
  6. Nanyang Technological University
  7. Singapore-France Merlion
  8. [ANR-12-BSV6-0002]

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G-quadruplexes (G4) are polymorphic four-stranded structures formed by certain G-rich nucleic acids, with various biological roles. However, structural features dictating their formation and/or function in vivo are unknown. In S. cerevisiae, the pathological persistency of G4 within the CEB1 minisatellite induces its rearrangement during leading-strand replication. We now show that several other G4-forming sequences remain stable. Extensive mutagenesis of the CEB25 minisatellite motif reveals that only variants with very short (<= 4 nt) G4 loops preferentially containing pyrimidine bases trigger genomic instability. Parallel biophysical analyses demonstrate that shortening loop length does not change the monomorphic G4 structure of CEB25 variants but drastically increases its thermal stability, in correlation with the in vivo instability. Finally, bioinformatics analyses reveal that the threat for genomic stability posed by G4 bearing short pyrimidine loops is conserved in C. elegans and humans. This work provides a framework explanation for the heterogeneous instability behavior of G4-forming sequences in vivo, highlights the importance of structure thermal stability, and questions the prevailing assumption that G4 structures with short or longer loops are as likely to form in vivo.

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