4.7 Article

Degradable cationic polyesters via ring-opening copolymerization of valerolactones as nanocarriers for the gene delivery

Journal

BIOORGANIC CHEMISTRY
Volume 116, Issue -, Pages -

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.bioorg.2021.105299

Keywords

Non-viral gene vector; [12]aneN(3); Valerolactone; Degradable polyester; Gene transfection

Funding

  1. National Natural Science Foundation of China [21372032, 21778012]

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In this study, five polyesters were synthesized and modified to condense DNA into nanoparticles. Among them, B3a and B3d demonstrated strong DNA condensing capabilities and potential transfection efficiency in different cells.
The development of cationic polymers as non-viral gene vectors has been hurdled by their high toxicity, thus degradable and biocompatible polymers are urgently demanded. Herein, five polyesters (B3a-B3e) were synthesized based on the ring-opening copolymerization between alpha-allyl-8-valerolactone and 8-valerolactone derivatives decorated with alkyl or alkoxyl chains of different lengths, followed by the modification with 1,5,9-triazacyclododecyl ([12]aneN(3)) through thiolene click reactions. The five polyesters effectively condensed DNA into nanoparticles. Of them, B3a with a shorter alkyl chain and B3d with more positive charged units showed stronger DNA condensing performance and can completely retard the migration of DNA at N/P = 1.6 in the presence of DOPE. B3b/DOPE with a longer alkyl chain exhibited the highest transfection efficiency in HeLa cells with 1.8 times of 25 kDa PEI, while B3d/DOPE with more positive charged units exhibited highest transfection efficiency in A549 cells with 2.3 times of 25 kDa PEI. B3b/DOPE and B3d/DOPE successfully delivered pEGFP into zebrafish, which was superior to 25 kDa PEI (1.5 folds and 1.1 folds, respectively). The cytotoxicity measurements proved that the biocompatibility of these polyesters was better than 25 kDa PEI, due to their degradable property in acid environment. The results indicated that these cationic polyesters can be developed as potential non-viral gene vectors for DNA delivery.

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