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      New generation of plasmid backbones devoid of antibiotic resistance marker for gene therapy trials.

      Molecular Therapy
      Animals, Drug Resistance, Bacterial, genetics, Genetic Therapy, Genetic Vectors, Humans, Plasmids

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          Abstract

          Since it has been established that the injection of plasmid DNA can lead to an efficient expression of a specific protein in vivo, nonviral gene therapy approaches have been considerably improved, allowing clinical trials. However, the use of antibiotic resistance genes as selection markers for plasmid production raises safety concerns which are often pointed out by the regulatory authorities. Indeed, a horizontal gene transfer to patient's bacteria cannot be excluded, and residual antibiotic in the final product could provoke allergic reactions in sensitive individuals. A new generation of plasmid backbones devoid of antibiotic resistance marker has emerged to increase the safety profile of nonviral gene therapy trials. This article reviews the existing strategies for plasmid maintenance and, in particular, those that do not require the use of antibiotic resistance genes. They are based either on the complementation of auxotrophic strain, toxin-antitoxin systems, operator-repressor titration, RNA markers, or on the overexpression of a growth essential gene. Minicircles that allow removing of the antibiotic resistance gene from the initial vector will also be discussed. Furthermore, reported use of antibiotic-free plasmids in preclinical or clinical studies will be listed to provide a comprehensive view of these innovative technologies.

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          Author and article information

          Journal
          21878901
          3222533
          10.1038/mt.2011.182

          Chemistry
          Animals,Drug Resistance, Bacterial,genetics,Genetic Therapy,Genetic Vectors,Humans,Plasmids
          Chemistry
          Animals, Drug Resistance, Bacterial, genetics, Genetic Therapy, Genetic Vectors, Humans, Plasmids

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