4.7 Article

Systematic Study of Enzymatic Degradation and Plasmid DNA Complexation of Mucus Penetrating Star-Shaped Lysine/Sarcosine Polypept(o)ides with Different Block Arrangements

Journal

MACROMOLECULAR BIOSCIENCE
Volume 22, Issue 8, Pages -

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/mabi.202200175

Keywords

DNA polyplexes; enzymatic degradation; mucus penetration; polypept(o)ides; star polymers

Funding

  1. Science Foundation Ireland (SFI)
  2. European Regional Development Fund (ERDF) [13/RC/2073_2]
  3. European Union [883951]
  4. IReL
  5. Marie Curie Actions (MSCA) [883951] Funding Source: Marie Curie Actions (MSCA)

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8-arm star polypeptides consisting of cationic polylysine and hydrophilic polysarcosine blocks were synthesized. The enzymatic hydrolysis and disintegration of the polypeptides showed a strong dependence on structural arrangements. The polyplexes formed by the polypeptides were capable of complexing plasmid DNA, had sizes around or below 200 nm, and could transport through mucus.
8-Arm star polypep(o)ides comprising cationic polylysine and hydrophilic polysarcosine blocks with a degree of polymerization (DP) of 30 per block are synthesized. Two different block sequences with polylysine as the inner and polysarcosine as the outer block and vice versa are obtained in addition to a statistical copolymer. Analysis of the enzymatic hydrolysis by the proteolytic enzyme trypsin demonstrates a strong dependence on structural arrangements. While polypept(o)ide disintegration is detectible after 24 h by Size Exclusion Chromatography (SEC), significant hydrolysis of the lysine blocks is only monitored after 48 h by fluorescamine labeling of the produced lysine and clearly accelerated in structures with more accessible polylysine blocks. All structures are capable of complexing plasmid DNA and form gene nanomedicines at sizes around or below 200 nm as determined by Dynamic Light Scattering (DLS), Nanoparticle Tracking Analysis (NTA), and Transition Electron Microscopy (TEM). The polyplex formation is slightly enhanced for both block structures over the random copolypept(o)ide. Moreover, it is demonstrated that the polyplexes can transport through mucus. The results highlight the importance of structural control in compartmentalized polymeric gene vector candidates with hydrophilic domains for potential mucosal delivery.

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