Linking of Antitumor trans NHC-Pt(II) Complexes to G-Quadruplex DNA Ligand for Telomeric Targeting
详细信息 查看全文
- 作者:Jean-François Betzer ; Frédérick Nuter ; Mélanie Chtchigrovsky ; Florian Hamon ; Guillaume Kellermann ; Samar Ali ; Marie-Ange Calméjane ; Sylvain Roque ; Joël Poupon ; Thierry Cresteil ; Marie-Paule Teulade-Fichou ; Angela Marinetti ; Sophie Bombard
- 刊名:Bioconjugate Chemistry
- 出版年:2016
- 出版时间:June 15, 2016
- 年:2016
- 卷:27
- 期:6
- 页码:1456-1470
- 全文大小:762K
- 年卷期:0
- ISSN:1520-4812
文摘
G-quadruplex structures (G4) are promising anticancerous targets. A great number of small molecules targeting these structures have already been identified through biophysical methods. In cellulo, some of them are able to target either telomeric DNA and/or some sequences involved in oncogene promotors, both resulting in cancer cell death. However, only a few of them are able to bind to these structures G4 irreversibly. Here we combine within the same molecule the G4-binding agent PDC (pyridodicarboxamide) with a N-heterocyclic carbene–platinum complex NHC-Pt already identified for its antitumor properties. The resulting conjugate platinum complex NHC-Pt-PDC stabilizes strongly G-quadruplex structures in vitro, with affinity slightly affected as compared to PDC. In addition, we show that the new conjugate binds preferentially and irreversibly the quadruplex form of the human telomeric sequence with a profile in a way different from that of NHC-Pt thereby indicating that the platination reaction is oriented by stacking of the PDC moiety onto the G4-structure. In cellulo, NHC-Pt-PDC induces a significant loss of TRF2 from telomeres that is considerably more important than the effect of its two components alone, PDC and NHC-Pt, respectively.