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Literature DB >> 24349706

Microfluidic Assembly of Cationic-β-Cyclodextrin:Hyaluronic Acid-Adamantane Host:Guest pDNA Nanoparticles.

Aditya Kulkarni¹, Ross Verheul¹, Kyle Defrees¹, Christopher J Collins¹, Ryan A Schuldt¹, Alexander Vlahu¹, David H Thompson¹.

Abstract

Traditionally, transfection complexes are typically formed by bulk mixing, producing particles with high polydispersity and limited control over vector size. Herein, we demonstrate the use of a commercial micro-reactor to assemble pDNA:cationic cyclodextrin:pendant polymer nanoparticles using a layer-by-layer approach. Our studies reveal that the particles formulated via microfluidic assembly have much smaller sizes, lower polydispersity, lower ζ-potentials, and comparable cell viability and transfection profiles in HeLa cells than bulk mixed particles. The complexes also show a flow rate-dependent stability, with particles formed at slower flow rates giving rise to more stable complexes as determined by heparin challenge. Our findings suggest that microfluidic reactors offer an attractive method for assembling reproducible, size-controlled complexes from multi-component transfection complex assemblies.

Entities: CellLine Chemical Disease Gene

Year: 2013 PMID： 24349706 PMCID： PMC3859440 DOI： 10.1039/C3BM00189J

Source DB: PubMed Journal: Biomater Sci ISSN： 2047-4830 Impact factor: 6.843

31 in total

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3 in total