Immune responses, not promoter inactivation, are responsible for decreased long-term expression following plasmid gene transfer into skeletal muscle

K. E. Wells; J. Maule; R. Kingston; K. Foster; J. McMahon; E. Damien; A. Poole; D. J. Wells

doi:10.1016/S0014-5793(97)00329-3

Immune responses, not promoter inactivation, are responsible for decreased long-term expression following plasmid gene transfer into skeletal muscle

K. E. Wells, J. Maule, R. Kingston, K. Foster, J. McMahon, E. Damien, A. Poole, D. J. Wells

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

48 Citations (Scopus)

Abstract

Long-term high-level in vivo gene expression appears to depend on the promoter chosen to drive the gene of choice. In many cases the promoter appears to 'switch off' some time after in vivo gene transfer. We demonstrate that, following intramuscular injection of β-galactosidase reporter plasmids, promoter 'switch off' is due to elimination of fibres expressing the transferred reporter gene by activation of a Th1 (cytotoxic) immune response. This finding, in the absence of stimulation of the immune system by viral vector proteins, has implications not only for gene transfer experiments but for the future of muscle-directed gene therapy.

Original language	English
Pages (from-to)	164-168
Number of pages	5
Journal	FEBS Letters
Volume	407
Issue number	2
DOIs	https://doi.org/10.1016/S0014-5793(97)00329-3
Publication status	Published - 28 Apr 1997
Externally published	Yes

Keywords

Cytotoxic T-cells
Gene therapy
Immunology
Plasmid DNA
Skeletal muscle

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10.1016/S0014-5793(97)00329-3

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abstract = "Long-term high-level in vivo gene expression appears to depend on the promoter chosen to drive the gene of choice. In many cases the promoter appears to 'switch off' some time after in vivo gene transfer. We demonstrate that, following intramuscular injection of β-galactosidase reporter plasmids, promoter 'switch off' is due to elimination of fibres expressing the transferred reporter gene by activation of a Th1 (cytotoxic) immune response. This finding, in the absence of stimulation of the immune system by viral vector proteins, has implications not only for gene transfer experiments but for the future of muscle-directed gene therapy.",

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AU - Wells, K. E.

AU - Maule, J.

AU - Kingston, R.

AU - Foster, K.

AU - McMahon, J.

AU - Damien, E.

AU - Poole, A.

AU - Wells, D. J.

PY - 1997/4/28

Y1 - 1997/4/28

N2 - Long-term high-level in vivo gene expression appears to depend on the promoter chosen to drive the gene of choice. In many cases the promoter appears to 'switch off' some time after in vivo gene transfer. We demonstrate that, following intramuscular injection of β-galactosidase reporter plasmids, promoter 'switch off' is due to elimination of fibres expressing the transferred reporter gene by activation of a Th1 (cytotoxic) immune response. This finding, in the absence of stimulation of the immune system by viral vector proteins, has implications not only for gene transfer experiments but for the future of muscle-directed gene therapy.

AB - Long-term high-level in vivo gene expression appears to depend on the promoter chosen to drive the gene of choice. In many cases the promoter appears to 'switch off' some time after in vivo gene transfer. We demonstrate that, following intramuscular injection of β-galactosidase reporter plasmids, promoter 'switch off' is due to elimination of fibres expressing the transferred reporter gene by activation of a Th1 (cytotoxic) immune response. This finding, in the absence of stimulation of the immune system by viral vector proteins, has implications not only for gene transfer experiments but for the future of muscle-directed gene therapy.

KW - Cytotoxic T-cells

KW - Gene therapy

KW - Immunology

KW - Plasmid DNA

KW - Skeletal muscle

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EP - 168

JO - FEBS Letters

JF - FEBS Letters

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ER -

Immune responses, not promoter inactivation, are responsible for decreased long-term expression following plasmid gene transfer into skeletal muscle

Abstract

Keywords

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