DNA Ministrings: Highly Safe and Effective Gene Delivery Vectors

Abstract

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Conventional plasmid DNA vectors play a significant role in gene therapy, but they also have considerable limitations: they can elicit adverse immune responses because of bacterial sequences they contain for maintenance and amplification in prokaryotes, their bioavailability is compromised because of their large molecular size, and they may be genotoxic. We constructed an in vivo platform to produce ministring DNA—mini linear covalently closed DNA vectors—that are devoid of unwanted bacterial sequences and encode only the gene(s) of interest and necessary eukaryotic expression elements. Transfection of rapidly and slowly dividing human cells with ministring DNA coding for enhanced green fluorescent protein resulted in significantly improved transfection, bioavailability, and cytoplasmic kinetics compared with parental plasmid precursors and isogenic circular covalently closed DNA counterparts. Ministring DNA that integrated into the genome of human cells caused chromosomal disruption and apoptotic death of possibly oncogenic vector integrants; thus, they may be safer than plasmid and circular DNA vectors.

Keywords

• bacterial sequence-free DNA vectors
• bacteriophage PY54 Tel/pal recombination system
• DNA vaccines
• gene therapy
• genotoxicity
• insertional oncogenesis
• intercellular kinetics
• MIDGE
• minicircle DNA
• ministring DNA
• plasmid DNA vector
• vector safety