Publications by authors named "J Dejeu"

Article Synopsis
  • i-Motifs (iMs) are unconventional DNA structures that form in cytosine-rich sequences, primarily under acidic conditions, and have gained attention due to the development of a specific antibody, iMab, which aids in their study in live cells.
  • Research shows that the interaction between iMab and cytosine-rich oligonucleotides relies on having at least two consecutive cytosines and is more pronounced in acidic pH, regardless of whether the sequence can form an iM structure.
  • Bulk-FRET experiments indicate that iMab can cause the unfolding of iM structures and binds to segments of 2-3 cytosines in single-stranded DNA, suggesting that findings using this antibody
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G-quadruplex DNA structures (G4) are proven to interfere with most genetic and epigenetic processes. Small molecules binding these structures (G4 ligands) are invaluable tools to probe G4-biology and address G4-druggability in various diseases (cancer, viral infections). However, the large number of reported G4 ligands (>1000) could lead to confusion while selecting one for a given application.

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Lectins are important biological tools for binding glycans, but recombinant protein expression poses challenges for some lectin classes, limiting the pace of discovery and characterization. To discover and engineer lectins with new functions, workflows amenable to rapid expression and subsequent characterization are needed. Here, we present bacterial cell-free expression as a means for efficient, small-scale expression of multivalent, disulfide bond-rich, rhamnose-binding lectins.

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Detecting cancer at the early stage of the disease is crucial to keep the best chance for successful treatment. The recent development of genomic screening, a methodology that is addressed to asymptomatic patients presumably at risk of carcinogenesis, has stimulated the quest for new tools able to signal the level of risk. Carcinogenesis has been associated to chronic oxidative stress exceeding the antioxidant defenses and leading to critical genome alteration levels.

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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 has been reported to modulate gene expression by stabilizing an i-motif structure in its promoter.

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