Literature DB >> 21893178

Reducible HPMA-co-oligolysine copolymers for nucleic acid delivery.

Julie Shi1, Russell N Johnson, Joan G Schellinger, Peter M Carlson, Suzie H Pun.   

Abstract

Biodegradability can be incorporated into cationic polymers via use of n>an class="Chemical">disulfide linkages that are degraded in the reducing environment of the cell cytosol. In this work, N-(2-hydroxypropyl)methacrylamide (HPMA) and methacrylamido-functionalized oligo-l-lysine peptide monomers with either a non-reducible 6-aminohexanoic acid (AHX) linker or a reducible 3-[(2-aminoethyl)dithiol] propionic acid (AEDP) linker were copolymerized via reversible addition-fragmentation chain transfer (RAFT) polymerization. Both of the copolymers and a 1:1 (w/w) mixture of copolymers with reducible and non-reducible peptides were complexed with DNA to form polyplexes. The polyplexes were tested for salt stability, transfection efficiency, and cytotoxicity. The HPMA-oligolysine copolymer containing the reducible AEDP linkers was less efficient at transfection than the non-reducible polymer and was prone to flocculation in saline and serum-containing conditions, but was also not cytotoxic at charge ratios tested. Optimal transfection efficiency and toxicity were attained with mixed formulation of copolymers. Flow cytometry uptake studies indicated that blocking extracellular thiols did not restore transfection efficiency and that the decreased transfection of the reducible polyplex is therefore not primarily caused by extracellular polymer reduction by free thiols. The decrease in transfection efficiency of the reducible polymers could be partially mitigated by the addition of low concentrations of EDTA to prevent metal-catalyzed oxidation of reduced polymers. Copyright Â
© 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 21893178      PMCID: PMC3240689          DOI: 10.1016/j.ijpharm.2011.08.015

Source DB:  PubMed          Journal:  Int J Pharm        ISSN: 0378-5173            Impact factor:   5.875


  46 in total

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6.  Purification of polyethylenimine polyplexes highlights the role of free polycations in gene transfer.

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8.  Effects of intermolecular thiol-disulfide interchange reactions on bsa fouling during microfiltration.

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9.  In vitro cytotoxicity testing of polycations: influence of polymer structure on cell viability and hemolysis.

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  9 in total

1.  The transduction of Coxsackie and Adenovirus Receptor-negative cells and protection against neutralizing antibodies by HPMA-co-oligolysine copolymer-coated adenovirus.

Authors:  Chung-Huei K Wang; Leslie W Chan; Russell N Johnson; David S H Chu; Julie Shi; Joan G Schellinger; André Lieber; Suzie H Pun
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2.  Application of living free radical polymerization for nucleic acid delivery.

Authors:  David S H Chu; Joan G Schellinger; Julie Shi; Anthony J Convertine; Patrick S Stayton; Suzie H Pun
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3.  Cathepsin B-sensitive polymers for compartment-specific degradation and nucleic acid release.

Authors:  David S H Chu; Russell N Johnson; Suzie H Pun
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Review 4.  Design of smart HPMA copolymer-based nanomedicines.

Authors:  Jiyuan Yang; Jindřich Kopeček
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5.  Optimization of Tet1 ligand density in HPMA-co-oligolysine copolymers for targeted neuronal gene delivery.

Authors:  David S H Chu; Joan G Schellinger; Michael J Bocek; Russell N Johnson; Suzie H Pun
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6.  Overcoming nonviral gene delivery barriers: perspective and future.

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7.  Optimization of brush-like cationic copolymers for nonviral gene delivery.

Authors:  Hua Wei; Joshuel A Pahang; Suzie H Pun
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8.  Comparative study of guanidine-based and lysine-based brush copolymers for plasmid delivery.

Authors:  Peter M Carlson; Joan G Schellinger; Joshuel A Pahang; Russell N Johnson; Suzie H Pun
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9.  Engineering biodegradable and multifunctional peptide-based polymers for gene delivery.

Authors:  Julie Shi; Joan G Schellinger; Suzie H Pun
Journal:  J Biol Eng       Date:  2013-10-24       Impact factor: 4.355

  9 in total

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