Abstract EN:

We have studied triplex-forming oligonucleotides (TFO), chemically modified as Locked Nucleic Acids (LNA), the TFO/LNA: 1/ Anti-gene properties TFO/LNA are able to form highly stable and specific complexes on the DNA target sequence in vitro. This thermodynamic stability leads to stable triplex formation in cells. 2/ Binding in the chromatine structure We have characterized TFO/LNA binding in chromatin and evaluated the cellular factors driving binding efficiency. We have shown that about 50% of the chromosomal target can be covered by the TFO specifically, and that the efficiency of TFO binding in chromatin was correlated to chromatin accessibility: TFO did bind more efficiently to unfolded chromatin regions. 3/ Induction of targeted DNA damages We have studied TFO covalently linked to a cleaving agent, the phenanthroline (OP). In cells, DNA modifications occur specifically at 50% of the episomal target plasmid. We are presently running experiments on chromosomally located target sites.