Antibiotic-Free Gene Vectors: A 25-Year Journey to Clinical Trials

Author:

Marie Corinne12ORCID,Scherman Daniel13

Affiliation:

1. Université Paris Cité, CNRS, Inserm, UTCBS, 75006 Paris, France

2. Chimie ParisTech, Université PSL, 75005 Paris, France

3. Fondation Maladies Rares, 75014 Paris, France

Abstract

Until very recently, the major use, for gene therapy, specifically of linear or circular DNA, such as plasmids, was as ancillary products for viral vectors’ production or as a genetic template for mRNA production. Thanks to targeted and more efficient physical or chemical delivery techniques and to the refinement of their structure, non-viral plasmid DNA are now under intensive consideration as pharmaceutical drugs. Plasmids traditionally carry an antibiotic resistance gene for providing the selection pressure necessary for maintenance in a bacterial host. Nearly a dozen different antibiotic-free gene vectors have now been developed and are currently assessed in preclinical assays and phase I/II clinical trials. Their reduced size leads to increased transfection efficiency and prolonged transgene expression. In addition, associating non-viral gene vectors and DNA transposons, which mediate transgene integration into the host genome, circumvents plasmid dilution in dividing eukaryotic cells which generate a loss of the therapeutic gene. Combining these novel molecular tools allowed a significantly higher yield of genetically engineered T and Natural Killer cells for adoptive immunotherapies due to a reduced cytotoxicity and increased transposition rate. This review describes the main progresses accomplished for safer, more efficient and cost-effective gene and cell therapies using non-viral approaches and antibiotic-free gene vectors.

Funder

European Commission

EC-DG research

E-RARE ERANET

European Union’s Seventh Framework Programme for research, technological development and demonstration

Publisher

MDPI AG

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