Application of Coiled Coil Peptides in Liposomal Anticancer Drug Delivery Using a Zebrafish Xenograft Model.

ACS Nano

Leiden Institute of Chemistry-Supramolecular and Biomaterial Chemistry, Leiden University, Einsteinweg 55, 2333CC Leiden, The Netherlands.

Published: August 2016

AI Article Synopsis

  • - The study investigates the use of coiled coil peptides E4 and K4, which can trigger liposomal membrane fusion, for targeted drug delivery applications, particularly to HeLa cells expressing K4.
  • - Researchers created E4-modified liposomes that successfully delivered the fluorescent dye and doxorubicin (DOX) to specific HeLa-K cells, showing greater effectiveness compared to free DOX.
  • - In vivo experiments in zebrafish models demonstrated that E4-liposomes could effectively deliver drugs to cancer cells, indicating their potential for enhanced selective targeting in clinical drug delivery systems.

Article Abstract

The complementary coiled coil forming peptides E4 [(EIAALEK)4] and K4 [(KIAALKE)4] are known to trigger liposomal membrane fusion when tethered to lipid vesicles in the form of lipopeptides. In this study, we examined whether these coiled coil forming peptides can be used for drug delivery applications. First, we prepared E4 peptide modified liposomes containing the far-red fluorescent dye TO-PRO-3 iodide (E4-Lipo-TP3) and confirmed that E4-liposomes could deliver TP3 into HeLa cells expressing K4 peptide on the membrane (HeLa-K) under cell culture conditions in a selective manner. Next, we prepared doxorubicin-containing E4-liposomes (E4-Lipo-DOX) and confirmed that E4-liposomes could also deliver DOX into HeLa-K cells. Moreover, E4-Lipo-DOX showed enhanced cytotoxicity toward HeLa-K cells compared to free doxorubicin. To prove the suitability of E4/K4 coiled coil formation for in vivo drug delivery, we injected E4-Lipo-TP3 or E4-Lipo-DOX into zebrafish xenografts of HeLa-K. As a result, E4-liposomes delivered TP3 to the implanted HeLa-K cells, and E4-Lipo-DOX could suppress cancer proliferation in the xenograft when compared to nontargeted conditions (i.e., zebrafish xenograft with free DOX injection). These data demonstrate that coiled coil formation enables drug selectivity and efficacy in vivo. It is envisaged that these findings are a step forward toward biorthogonal targeting systems as a tool for clinical drug delivery.

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http://dx.doi.org/10.1021/acsnano.6b01410DOI Listing

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