Mucus altering agents as adjuncts for nonviral gene transfer to airway epithelium

S Ferrari; C Kitson; R Farley; R Steel; C Marriott; D A Parkins; M Scarpa; B Wainwright; M J Evans; W H Colledge; D M Geddes; E W F W Alton

doi:10.1038/sj.gt.3301525

Mucus altering agents as adjuncts for nonviral gene transfer to airway epithelium

S Ferrari, C Kitson, R Farley, R Steel, C Marriott, D A Parkins, M Scarpa, B Wainwright, M J Evans, W H Colledge, D M Geddes, E W F W Alton

King's College London

Research output: Contribution to journal › Article › peer-review

105 Citations (Scopus)

Abstract

Nonviral vectors have been shown to be a safe and valid alternative to recombinant viruses for gene therapy of cystic fibrosis (CF). Nevertheless, gene transfer efficiency needs to be increased before clinical efficacy is likely in man. One barrier to increased efficacy is normal airway mucus. Using an ex vivo model of sheep tracheal epithelium, we show that this barrier can, in part, be overcome by treatment with the mucolytic agents, Nacystelyn or N-acetylcysteine using either a cationic lipid or a cationic polymer as the gene transfer agent. Further, in vivo application of either Nacystelyn or the anticholinergic glycopyrrolate, both clinically used agents, resulted in increased reporter gene expression in the mouse lung, but no significant correction of the bioelectric defect in CF null mice. These results, whilst unlikely to be sufficient in themselves to achieve clinically relevant gene therapy, may be a further useful step in the attainment of this goal.

Original language	English
Pages (from-to)	1380 - 1386
Number of pages	7
Journal	Gene Therapy
Volume	8
Issue number	18
DOIs	https://doi.org/10.1038/sj.gt.3301525
Publication status	Published - 2001

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title = "Mucus altering agents as adjuncts for nonviral gene transfer to airway epithelium",

abstract = "Nonviral vectors have been shown to be a safe and valid alternative to recombinant viruses for gene therapy of cystic fibrosis (CF). Nevertheless, gene transfer efficiency needs to be increased before clinical efficacy is likely in man. One barrier to increased efficacy is normal airway mucus. Using an ex vivo model of sheep tracheal epithelium, we show that this barrier can, in part, be overcome by treatment with the mucolytic agents, Nacystelyn or N-acetylcysteine using either a cationic lipid or a cationic polymer as the gene transfer agent. Further, in vivo application of either Nacystelyn or the anticholinergic glycopyrrolate, both clinically used agents, resulted in increased reporter gene expression in the mouse lung, but no significant correction of the bioelectric defect in CF null mice. These results, whilst unlikely to be sufficient in themselves to achieve clinically relevant gene therapy, may be a further useful step in the attainment of this goal.",

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AU - Ferrari, S

AU - Kitson, C

AU - Farley, R

AU - Steel, R

AU - Marriott, C

AU - Parkins, D A

AU - Scarpa, M

AU - Wainwright, B

AU - Evans, M J

AU - Colledge, W H

AU - Geddes, D M

AU - Alton, E W F W

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AB - Nonviral vectors have been shown to be a safe and valid alternative to recombinant viruses for gene therapy of cystic fibrosis (CF). Nevertheless, gene transfer efficiency needs to be increased before clinical efficacy is likely in man. One barrier to increased efficacy is normal airway mucus. Using an ex vivo model of sheep tracheal epithelium, we show that this barrier can, in part, be overcome by treatment with the mucolytic agents, Nacystelyn or N-acetylcysteine using either a cationic lipid or a cationic polymer as the gene transfer agent. Further, in vivo application of either Nacystelyn or the anticholinergic glycopyrrolate, both clinically used agents, resulted in increased reporter gene expression in the mouse lung, but no significant correction of the bioelectric defect in CF null mice. These results, whilst unlikely to be sufficient in themselves to achieve clinically relevant gene therapy, may be a further useful step in the attainment of this goal.

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ER -

Mucus altering agents as adjuncts for nonviral gene transfer to airway epithelium

Abstract

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