Effect of intron A from human cytomegalovirus (Towne) immediate-early gene on heterologous expression in mammalian cells

Chapman, Barbara S.; Thayer, Richard M.; Vincent, Karen A.; Haigwood, Nancy L.

doi:10.1093/nar/19.14.3979

Cited by 283 publications

(164 citation statements)

References 50 publications

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“…As control groups, apoEdeficient mice were injected with pCMV5 empty plasmid or pRC112-HCV plasmid, coding for an unrelated foreign protein. 22,28 These control groups were used in order to exclude the possibility of a non-specific mechanism by which an immune response to the vector components or the foreign transgene results in a non-specific reduction in serum cholesterol. We showed that the appearance of apoE in the blood of apoE-deficient mice injected with pCMV-E3 was associated with a dramatic reduction of serum cholesterol levels, as compared with control mice.…”

Section: Discussionmentioning

confidence: 99%

“…11 As negative controls, the pCMV5 and pRC112-HCV plasmid vectors were used. 22,28 Plasmids were grown in Escherichia coli DH5 ␣ F1Ј and prepared as described elsewhere. 22 Animals and intramuscular injections C57BL/6J apoE-deficient mice were obtained from Jackson Laboratories (Bar Harbor, ME, USA) and were maintained on a normal chow diet.…”

Section: Plasmid Vectorsmentioning

confidence: 99%

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Treatment of severe hypercholesterolemia in apolipoprotein E-deficient mice by intramuscular injection of plasmid DNA

et al. 2000

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We report on systemic delivery and long-term biological effects of apolipoprotein E (apoE) obtained by intramuscular (i.m.) plasmid DNA injection. ApoE plays an important role in lipoprotein catabolism and apoE knock-out mice develop severe hypercholesterolemia and diffuse atherosclerosis. We have injected apoE-deficient mice with 80 g of a plasmid vector (pCMV-E3) encoding the human apoE3 cDNA under the control of the CMV promoter-enhancer in both posterior legs. Local expression of the transgene was demonstrated throughout 16 weeks. Human apoE3 recombinant protein reached 0.6 ng/ml serum level. After i.m. injection of pCMV-E3 expression vector the mean serum cholesterol concentrations decreased from 439 ± 57 mg/dl to 253 ± 99 mg/dl (P Ͻ 0.05) 2 weeks after injection and persisted at a

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Section: Discussionmentioning

confidence: 99%

Section: Plasmid Vectorsmentioning

confidence: 99%

Treatment of severe hypercholesterolemia in apolipoprotein E-deficient mice by intramuscular injection of plasmid DNA

et al. 2000

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“…1,2 Cytokine gene therapy approaches have been actively evaluated for a variety of potential applications in the fields of cancer immunotherapy, cancer vaccines and gene-based vaccinations against infectious diseases. [3][4][5][6][7][8][9] For many cytokine gene therapy approaches, a sharp transient gene expression peak, rather than a high and prolonged transgenic cytokine expression is valued by investigators. [3][4][5][6][7][8][9][10][11] It has also been suggested that although using current transgenic experimental systems results in low specific transgenic cytokine levels in regional or localized tissue, a 10-20 fold increase in expression levels might effectively facilitate certain physiological activities and an efficacious response, as indicated in some tumor vaccine studies.…”

Section: Introductionmentioning

confidence: 99%

“…[3][4][5][6][7][8][9] For many cytokine gene therapy approaches, a sharp transient gene expression peak, rather than a high and prolonged transgenic cytokine expression is valued by investigators. [3][4][5][6][7][8][9][10][11] It has also been suggested that although using current transgenic experimental systems results in low specific transgenic cytokine levels in regional or localized tissue, a 10-20 fold increase in expression levels might effectively facilitate certain physiological activities and an efficacious response, as indicated in some tumor vaccine studies. 12,13 Taking into consideration the aforementioned advantages of increasing transgene expression and the necessary caution of not 'overdosing' gene transfer vectors due to safety concerns, we believe that it is very important to start developing specific transgene expression systems that can be augmented by molecular biology strategies for upgrading gene expression levels.…”

Section: Introductionmentioning

confidence: 99%

“…In this experiment, cytokine genes were constructed to contain a CMV immediate/early promoter sequence 4 with either a CMV-derived intron A sequence or a short, SV40-derived splice donor/splice acceptor (SD/SA) sequence. Alternatively, cytokine transgenes were constructed under the control of a human EF-1a promoter linked with an SV40 intron-1 enhancer.…”

Section: Effects Of CMV Promoter/intron a And Ef-1a Promoter/intron 1mentioning

confidence: 99%

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Molecular strategies for improving cytokine transgene expression in normal and malignant tissues

Turner

2003

Gene Ther

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The augmentation and optimization of specific targeted transgene expression systems are important strategies for clinical research into gene therapy and DNA vaccination, due to safety considerations. In this study, we introduced 3 0 untranslated regions and transcriptional control modifications and direct tandem or combinational vector design strategies into a number of specific cytokine cDNA expression plasmids. The experiments were performed in parallel using both in vivo and in vitro transgene expression systems. In vivo studies were carried out using gene gun delivery of test vectors into mouse skin tissues. A combination of specific cell lines and fresh cell explants were used for in vitro and ex vivo transgene expression assay systems. The results from these comparative experiments demonstrated that a number of molecular biology manipulations can be readily adapted to define and significantly enhance the level or/and duration of transgene expression for a group of clinically relevant cytokine genes, with very similar effects for both in vivo and in vitro test systems. This cytokine transgene expression system may offer a favorable means for improving the efficiency of cytokine gene therapy and DNA vaccines in future clinical studies.

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DNA vaccines: Vector design, delivery, and antigen presentation

Feltquate¹

1998

J. Cell. Biochem.

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Inoculations with antigen-expressing plasmid DNAs (DNA vaccines) in the production of protective immune responses. Since the initial development of DNA vaccines more than 5 years ago, major strides have been made in the design of efficient vaccine vectors and in the process of vaccine delivery. However, many questions remain regarding the mechanism of cellular transfection and in the development of immune responses. This review addresses functional aspects of DNA vaccines, including vector design and delivery, as well as cellular transfection and antigen presentation. J. Cell. Biochem. Suppls. 30/31:304-311, 1998. © 1998 Wiley-Liss, Inc.

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Effect of intron A from human cytomegalovirus (Towne) immediate-early gene on heterologous expression in mammalian cells

Cited by 283 publications

References 50 publications

Treatment of severe hypercholesterolemia in apolipoprotein E-deficient mice by intramuscular injection of plasmid DNA

Treatment of severe hypercholesterolemia in apolipoprotein E-deficient mice by intramuscular injection of plasmid DNA

Molecular strategies for improving cytokine transgene expression in normal and malignant tissues

DNA vaccines: Vector design, delivery, and antigen presentation

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