PLoS ONE (Jan 2024)

Quadruplex-duplex junction in LTR-III: A molecular insight into the complexes with BMH-21, namitecan and doxorubicin.

  • Stefania Mazzini,
  • Gigliola Borgonovo,
  • Salvatore Princiotto,
  • Roberto Artali,
  • Loana Musso,
  • Anna Aviñó,
  • Ramon Eritja,
  • Raimundo Gargallo,
  • Sabrina Dallavalle

DOI
https://doi.org/10.1371/journal.pone.0306239
Journal volume & issue
Vol. 19, no. 7
p. e0306239

Abstract

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Quadruplex-Duplex (Q-D) junctions are unique structural motifs garnering increasing interest as drug targets, due to their frequent occurrence in genomic sequences. The viral HIV LTR-III sequence was chosen as a Q-D junction model to study the affinity of the selected compounds BMH-21, namitecan (ST-1968), and doxorubicin (DOXO), all containing a planar polycyclic aromatic moiety, linked to either one short aminoalkyl or an aminoglycosyl group. A multidisciplinary approach that combines NMR spectroscopy, molecular modelling, circular dichroism (CD) and fluorescence spectroscopy was employed. The studied ligands induced moderate but clear stabilization to the Q-D junction by interacting with the interfacial tetrad. DOXO was found to be the best Q-D junction binder. Interestingly, the removal of the aminoglycosyl group significantly changed the pattern of the interactions, indicating that highly polar substituents have a stronger affinity with the exposed regions of the Q-D junction, particularly at the level of the interfacial tetrad.