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Novel Synthesis of IMC-48 and Affinity Evaluation with Different i-Motif DNA Sequences.

Florian BerthiolJoseph BoissierasHugues BonnetMarie PierrotChristian PhilouzeJean-François PoissonAnton GranzhanJérôme DejeuEric Defrancq
Published in: Molecules (Basel, Switzerland) (2023)
During the last decade, the evidence for the biological relevance of i-motif DNA (i-DNA) has been accumulated. However, relatively few molecules were reported to interact with i-DNA, and a controversy concerning their binding mode, affinity, and selectivity persists in the literature. In this context, the cholestane derivative IMC-48 has been reported to modulate bcl-2 gene expression by stabilizing an i-motif structure in its promoter. In the present contribution, we report on a novel, more straightforward, synthesis of IMC-48 requiring fewer steps compared to the previous approach. Furthermore, the interaction of IMC-48 with four different i-motif DNA sequences was thoroughly investigated by bio-layer interferometry (BLI) and circular dichroism (CD) spectroscopy. Surprisingly, our results show that IMC-48 is a very weak ligand of i-DNA as no quantifiable interaction or significant stabilization of i-motif structures could be observed, stimulating a quest for an alternative mechanism of its biological activity.
Keyphrases
  • circulating tumor
  • single molecule
  • cell free
  • gene expression
  • systematic review
  • nucleic acid
  • high resolution
  • circulating tumor cells