Development of a Langerhans cell-targeted gene therapy format using a dendritic cell-specific promoter

被引:0
|
作者
A Morita
K Ariizumi
R Ritter III
JV Jester
T Kumamoto
SA Johnston
A Takashima
机构
[1] University of Texas Southwestern Medical Center,Department of Dermatology
[2] University of Texas Southwestern Medical Center,Department of Ophthalmology
[3] Center for Biomedical Invention,undefined
[4] University of Texas Southwestern Medical Center,undefined
来源
Gene Therapy | 2001年 / 8卷
关键词
Langerhans cells; dendritic cells; gene gun; transcriptional regulation; dectin-2 promoter;
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学科分类号
摘要
Langerhans cells (LC), which are a skin-specific member of the dendritic cell (DC) family of antigen presenting cells, play critical roles in the initiation of cellular immune responses in the skin. We developed a LC-targeted gene therapy format in this study, aimed at the establishment of in situ protocols for genetic manipulation of LC function. Dectin-2 is a unique C-type lectin that is expressed selectively by DC, including epidermal LC. A 3.2 kb 5′ flanking fragment isolated from the mouse dectin-2 gene, termed the dectin-2 promoter (pDec2), exhibited significant transcriptional activities in epidermal-derived DC lines of the XS series, but not in any of the tested non-DC lines. When pDec2-driven luciferase gene (pDec2-Luc) or enhanced green fluorescence protein gene (pDec2-EGFP) was delivered to mouse skin using the gene gun, expression of the corresponding gene product was observed in the epidermal compartment almost exclusively by the IA+ population (ie LC). LC in the gene gun-treated sites showed features of mature DC and they migrated to the draining lymph node, suggesting that LC-targeted gene expression may lead to the development of immune responses. In fact, EGFP-specific cellular immune responses became detectable after gene gun-mediated delivery of pDec2-EGFP plasmid. These results introduce a new concept that LC function can be genetically manipulated in situ by the combination of gene gun-mediated DNA delivery and a DC-specific promoter.
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页码:1729 / 1737
页数:8
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