Pharmaceutics (Feb 2023)

Elastin-Derived VGVAPG Fragment Decorated Cell-Penetrating Peptide with Improved Gene Delivery Efficacy

  • Wen-Juan Shen,
  • Duo-Mei Tian,
  • Le Fu,
  • Biao Jin,
  • Yu Liu,
  • Yun-Sheng Xu,
  • Yong-Bin Ye,
  • Xiao-Bo Wang,
  • Xiao-Jun Xu,
  • Chun Tang,
  • Fang-Ping Li,
  • Chun-Fei Wang,
  • Gang Wu,
  • Le-Ping Yan

DOI
https://doi.org/10.3390/pharmaceutics15020670
Journal volume & issue
Vol. 15, no. 2
p. 670

Abstract

Read online

Cell-penetrating peptides (CPPs) are attractive non-viral gene delivery vectors due to their high transfection capacity and safety. Previously, we have shown that cell-penetrating peptide RALA can be a promising gene delivery vector for chronic wound regeneration application. In this study, we engineered a novel peptide called RALA-E by introducing elastin-derived VGVAPG fragment into RALA, in order to target the elastin-binding protein on the cell surface and thus improve delivery efficacy of RALA. The transfection efficiency of RALA-E was evaluated by transfecting the HEK-293T and HeLa cell lines cells with RALA-E/pDNA complexes and the flow-cytometry results showed that RALA-E significantly increased the transfection efficiency by nearly 20% in both cell lines compared to RALA. Inhibition of pDNA transfection on HEK-293T cells via chlorpromazine, genistein and mβCD showed that the inhibition extent in transfection efficiency was much less for RALA-E group compared to RALA group. In addition, RALA-E/miR-146a complexes showed up to 90% uptake efficiency in macrophages, and can escape from the endosome and enter the nucleus to inhibit the expression of inflammation genes. Therefore, the developed RALA-E peptide has high potential as a safe and efficient vector for gene therapy application.

Keywords