4.7 Article

Cationic Polymer Intercalation into the Lipid Membrane Enables Intact Polyplex DNA Escape from Endosomes for Gene Delivery

Journal

MOLECULAR PHARMACEUTICS
Volume 13, Issue 6, Pages 1967-1978

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.6b00139

Keywords

gene therapy; gene delivery; polyplexes; polyplex-cell membrane interactions; membrane intercalation; linear poly(ethylenimine); molecular beacon; FRET molecular beacon

Funding

  1. Federal funds from the National Institutes of Health, National Institute of Biomedical Imaging and Bioengineering [EB005028]

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Developing improved cationic polymer-DNA polyplexes for gene delivery requires improved understanding of DNA transport from endosomes into the nucleus. Using a FRET-capable oligonucleotide molecular beacon (OMB), we monitored the transport of intact DNA to cell organelles. We observed that for effective (jetPEI) and ineffective (G5 PAMAM) vectors, the fraction of cells displaying intact OMB in the cytosol (jetPEI >> GS PAMAM) quantitatively predicted the fraction expressing transgene (jetPEI >> G5 PAMAM). Intact OMB delivered with PAMAM and confined to endosomes could be released to the cytosol by the subsequent addition of L-PEI, with a corresponding 10-fold increase in transgene expression. These results suggest that future vector development should optimize vectors for intercalation into, and destabilization of, the endosomal membrane. Finally, the study highlights a two-step strategy in which the pDNA is loaded in cells using one vector and endosomal release is mediated by a second agent.

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