Low dose and gene gun immunization with a hepatitis C virus nonstructural (NS) 3 DNA-based vaccine containing NS4A inhibit NS3/4A-expressing tumors in vivo

被引:0
|
作者
L Frelin
M Alheim
A Chen
J Söderholm
B Rozell
C Barnfield
P Liljeström
M Sällberg
机构
[1] F 68,Division of Clinical Virology
[2] Karolinska Institutet at Huddinge University Hospital,Division of Pathology and Clinical Research Centre
[3] Karolinska Institutet at Huddinge University Hospital,undefined
[4] Swedish Institute for Infectious Disease Control,undefined
[5] Microbiology and Tumourbiology Centre,undefined
[6] Karolinska Institutet,undefined
来源
Gene Therapy | 2003年 / 10卷
关键词
hepatitis C virus; HCV; NS3; DNA vaccine; gene gun;
D O I
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学科分类号
摘要
The hepatitis C virus (HCV) protease and helicase encompasses the nonstructural (NS) 3 protein and the cofactor NS4A, which targets the NS3/4A-complex to intracellular membranes. We here evaluate the importance of NS4A in NS3-based genetic immunogens. A full-length genotype 1 NS3/4A gene was cloned into a eucaryotic expression vector in the form of NS3/4A and NS3 alone. Transient transfections revealed that the inclusion of NS4A increased the expression levels of NS3. Subsequently, immunization with the NS3/4A gene primed 10- to 100-fold higher levels of NS3-specific antibodies as compared to immunization with the NS3 gene. Humoral responses primed by the NS3/4A gene had a higher IgG2a/IgG1 ratio (>20) as compared to the NS3 gene (3.0), suggesting a T helper 1-skewed response. Low dose i.m. (10 μg) immunization with the NS3/4A gene inhibited the growth of NS3/4A-expressing tumor cells in vivo, whereas the NS3 gene alone or NS3 protein did not. We then evaluated the efficiency of the NS3/4A gene administered by the gene gun, at the same doses used for humans, in priming cytotoxic T lymphocyte (CTL) responses. Three to four 4 μg doses of the NS3/4A gene primed CTL at a precursor frequency of 2–4%, which inhibited the growth of NS3/4A-expressing tumor cells in vivo. Thus, NS4A enhances the expression levels and immunogenicity of NS3, and an NS3/4A gene delivered transdermally could be a therapeutic vaccine candidate.
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页码:686 / 699
页数:13
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