Abstract
The transient delivery of gene products (RNA or proteins) is not a biotechnological invention but rather an evolutionarily conserved process underlying and regulating a variety of biological functions. On the basis of insights into the underlying mechanisms, several viral and cell-based approaches have been developed for the delivery of RNA or proteins. Prominent applications include the induction of major biological or therapeutic effects on the basis of “hit-and-run” mechanisms, such as vaccination, cell fate modification (reprogramming, differentiation), control of cell trafficking, enhancement of cell regeneration, and genome engineering using sequence-specific recombinases or nucleases. Ideally, procedures for delivery of RNA or proteins should be targeted to specific cells, overcome biophysical hurdles without harming cellular integrity, circumvent the various alarm signals of the innate immune system, allow dose-controlled delivery of functional biomacromolecules, and avoid the induction of an adaptive immune response. Here we review the current state of approaches for the delivery of mRNA and proteins with a focus on RNA viruses, virus-like particles including retrovirus particle-mediated transfer of mRNA or proteins, extracellular vesicles, and cell-penetrating peptides. The basic concepts and recent advances are put into perspective in the context of potential limitations of the technologies and strategies to overcome cellular barriers and defense mechanisms.
Keywords: cell-penetrating peptide, gene therapy, microvesicle, protein transduction, RNA transfer, transient delivery, viral vector, virus-like particle, biomacromolecules, recombinases
Current Gene Therapy
Title: Viral and Non-Viral Approaches for Transient Delivery of mRNA and Proteins
Volume: 11 Issue: 5
Author(s): Juliane W. Schott, Melanie Galla, Tamaryin Godinho, Christopher Baum and Axel Schambach
Affiliation:
Keywords: cell-penetrating peptide, gene therapy, microvesicle, protein transduction, RNA transfer, transient delivery, viral vector, virus-like particle, biomacromolecules, recombinases
Abstract: The transient delivery of gene products (RNA or proteins) is not a biotechnological invention but rather an evolutionarily conserved process underlying and regulating a variety of biological functions. On the basis of insights into the underlying mechanisms, several viral and cell-based approaches have been developed for the delivery of RNA or proteins. Prominent applications include the induction of major biological or therapeutic effects on the basis of “hit-and-run” mechanisms, such as vaccination, cell fate modification (reprogramming, differentiation), control of cell trafficking, enhancement of cell regeneration, and genome engineering using sequence-specific recombinases or nucleases. Ideally, procedures for delivery of RNA or proteins should be targeted to specific cells, overcome biophysical hurdles without harming cellular integrity, circumvent the various alarm signals of the innate immune system, allow dose-controlled delivery of functional biomacromolecules, and avoid the induction of an adaptive immune response. Here we review the current state of approaches for the delivery of mRNA and proteins with a focus on RNA viruses, virus-like particles including retrovirus particle-mediated transfer of mRNA or proteins, extracellular vesicles, and cell-penetrating peptides. The basic concepts and recent advances are put into perspective in the context of potential limitations of the technologies and strategies to overcome cellular barriers and defense mechanisms.
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Cite this article as:
W. Schott Juliane, Galla Melanie, Godinho Tamaryin, Baum Christopher and Schambach Axel, Viral and Non-Viral Approaches for Transient Delivery of mRNA and Proteins, Current Gene Therapy 2011; 11 (5) . https://dx.doi.org/10.2174/156652311797415872
DOI https://dx.doi.org/10.2174/156652311797415872 |
Print ISSN 1566-5232 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5631 |
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