Co-delivery of anti-PLK-1 siRNA and camptothecin by nanometric polydiacetylenic micelles results in a synergistic cell killing

Manon Ripoll; Marie Pierdant; Patrick Neuberg; Dominique Bagnard; Alain Wagner; Antoine Kichler; Jean-Serge Remy

doi:10.1039/c8ra03375g

Co-delivery of anti-PLK-1 siRNA and camptothecin by nanometric polydiacetylenic micelles results in a synergistic cell killing

RSC Adv. 2018 Jun 6;8(37):20758-20763. doi: 10.1039/c8ra03375g. eCollection 2018 Jun 5.

Authors

Manon Ripoll¹, Marie Pierdant², Patrick Neuberg¹, Dominique Bagnard², Alain Wagner¹, Antoine Kichler¹, Jean-Serge Remy¹

Affiliations

¹ University of Strasbourg, CNRS, UMR7199, Labex Medalis, icFRC 67400 Illkirch France remy@unistra.fr.
² MN3T Lab, Fédération de Médecine Translationnelle, Labex Medalis, INSERM U1109, University of Strasbourg 67400 Illkirch France.

Abstract

Recently, it has been shown that the efficiency of antitumoral drugs can be enhanced when combined with therapeutic siRNAs. In the present study, an original platform based on polydiacetylenic micelles containing a cationic head group able to efficiently deliver a small interfering RNA (siRNA) targeting the PLK-1 gene while offering a hydrophobic environment for encapsulation of lipophilic drugs such as camptothecin is developed. We demonstrate that the co-delivery of these two agents with our micellar system results in a synergistic tumor cell killing of cervical and breast cancer cell lines in vitro. The combined drugs are active in a subcutaneous in vivo cancer model. Altogether, the results show that our nanometric micellar delivery system can be used for the development of new drug-siRNA combo-therapies.