Gene delivery of PEI incorporating with functional block copolymer via non-covalent assembly strategy

  • Yuling Hu
  • , Dezhong Zhou
  • , Congxin Li
  • , Hao Zhou
  • , Jiatong Chen
  • , Zhengpu Zhang
  • , Tianying Guo

Research output: Contribution to journalArticlepeer-review

32 Scopus citations

Abstract

A novel functional diblock polymer P(PEGMA-b-MAH) is prepared and incorporated to improve the gene delivery efficiency of poly(ethyleneimine) PEI via non-covalent assembly strategy. First, P(PEGMA-b-MAH) is prepared from l-methacrylamidohistidine methyl ester (MAH) by reversible addition fragmentation chain transfer polymerization, with poly[poly(ethylene glycol) methyl ether methacrylate] (P(PEGMA)) as the macroinitiator. Then P(PEGMA-b-MAH) is assembled with plasmid DNA (pDNA) and PEI (Mw = 10 kDa) to form PEI/P(PEGMA-b-MAH)/pDNA ternary complexes. The agarose gel retardation assay shows that the presence of P(PEGMA-b-MAH) does not interfere with DNA condensation by the PEI. Dynamic light scattering tests show that PEI/P(PEGMA-b-MAH)/pDNA ternary complexes have excellent serum stability. In vitro transfection indicates that, compared to the P(PEGMA-b-MAH) free PEI-25k/pDNA binary complexes, PEI-10k/P(PEGMA-b-MAH)/pDNA ternary complexes have lower cytotoxicity and higher gene transfection efficiency, especially under serum conditions. The ternary complexes proposed here can inspire a new strategy for the development of gene and drug delivery vectors.

Original languageEnglish
Pages (from-to)5003-5012
Number of pages10
JournalActa Biomaterialia
Volume9
Issue number2
DOIs
StatePublished - Feb 2013
Externally publishedYes

Keywords

  • Functional diblock copolymer
  • Gene vector
  • Poly(ethyleneimine)
  • Ternary complexes

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