Transfection and Physical Properties of Various Saccharide, Poly(ethylene Glycol), and Antibody-derivatized Polyethylenimines (PEI)
Overview
Molecular Biology
Affiliations
Background: The ideal non-viral vector should be cell-type directed and form complexes with DNA that are physically stable, small and electrically neutral.
Methods: We have synthesized several PEI derivatives that coat the PEI/DNA complexes with water-soluble residues able to stabilize the particles, to mask their surface charge and eventually to direct them to a particular tissue. The morphologies and sizes of the complexes were observed by TEM and DLS techniques, and their apparent surface charge was quantitated by zeta potential measurements; in vitro transfection efficacies were determined in serum-containing cell culture medium.
Results: When compared to DNA complexes formed with the unmodified PEI, extensive grafting with maltose (15-25% of the amine functions) led to beneficial electrostatic shielding of the particle surface, but was unable to prevent aggregation in physiological salt concentration. More extended hydrophilic residues were therefore explored as a mean of physical repulsion between the particles. Low grafting (2.7%) with a linear dextran non-asaccharide led to small and stable toroids having no apparent surface charge, yet still reaching effective transfection levels. Electron microscopy of complexes with a higher extent of grafting showed worm-like structures unsuited for cell entry. Conjugation of PEI with as little as 0.5% of a terminally galactose-derivatized polyethyleneglycol (PEG)-3400 also gave neutral complexes of another worm-like structure that failed to transfect receptor-expressing hepatocytes.
Conclusion: These results show that conjugation of large and flexible hydrophilic residues to PEI, while protecting the complexes from parasitic interactions also interfere with DNA condensation. PEG conjugation after PEI/DNA complex formation may avoid this problem, provided intracomplex reorganization is slow. Finally an anti-GD2 antibody (mAb) grafted with PEI was synthesized. The corresponding protein-coated DNA complexes were compact and small (50-60 nm), yet did not enhance transfection of GD2 ganglioside-expressing cells.
Peptide-Functionalized Dendrimer Nanocarriers for Targeted Microdystrophin Gene Delivery.
Hersh J, Condor Capcha J, Irion C, Lambert G, Noguera M, Singh M Pharmaceutics. 2021; 13(12).
PMID: 34959441 PMC: 8708248. DOI: 10.3390/pharmaceutics13122159.
Polymerized Albumin Receptor of Hepatitis B Virus for Evading the Reticuloendothelial System.
Takagi K, Somiya M, Jung J, Iijima M, Kuroda S Pharmaceuticals (Basel). 2021; 14(5).
PMID: 33923102 PMC: 8145202. DOI: 10.3390/ph14050408.
Calcium enhances polyplex-mediated transfection efficiency of plasmid DNA in Jurkat cells.
Ayyadevara V, Roh K Drug Deliv. 2020; 27(1):805-815.
PMID: 32489110 PMC: 8216448. DOI: 10.1080/10717544.2020.1770371.
Polyplex Evolution: Understanding Biology, Optimizing Performance.
Hall A, Lachelt U, Bartek J, Wagner E, Moein Moghimi S Mol Ther. 2017; 25(7):1476-1490.
PMID: 28274797 PMC: 5498806. DOI: 10.1016/j.ymthe.2017.01.024.
Unusual Salt and pH Induced Changes in Polyethylenimine Solutions.
Curtis K, Miller D, Millard P, Basu S, Horkay F, Chandran P PLoS One. 2016; 11(9):e0158147.
PMID: 27685846 PMC: 5042459. DOI: 10.1371/journal.pone.0158147.