中國醫藥大學機構典藏 China Medical University Repository, Taiwan:Item 310903500/31154
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    题名: AAV2-mediated interleukin-12 in the treatment of malignant brain tumors through activation of NK cells
    作者: (Tsung-Lang Chiu);林欣榮(Shinn-Zong Lin);(Wan-Hua Hsieh);(Chih-Wen Peng)
    贡献者: 醫學院免疫學研究所;中國附醫神經精神醫學中心;北港醫院神經外科
    日期: 2009-12
    上传时间: 2010-09-27 15:43:31 (UTC+8)
    摘要: Interleukin-12 has been elucidated as a powerful anti-cancer factor in pre-clinical research. However, the obstacles of this modality that emerged from human clinical trails included the toxicity of repeated large dose administration and short effective duration. Therefore, a prolonged, constant therapeutic level of interleukin-12 is required to reduce the adverse effects and enhance the therapeutic efficacy. In this study, 54 nude mice were divided into three groups treated with rAAV2 encoding interleukin-12, rAAV2 vector, and PBS, respectively. All nude mice received human glioblastoma multiforme cell line DBTRG implantation. The biochemistry studies included serum levels of interleukin-12, isotypes of immunoglobulin, interferon-γ, and TNF-α. The activated NK cells were sorted from the spleen by flow cytometry and the cytotoxicity of NK cells were evaluated by LDH assay. In the rAAV2 encoding interleukin-12 group, substantial expression of interleukin-12 was obtained with a serum level of 120-150 pg/ml through the experimental course and a significant increase of activated NK cells was achieved. The splenocytes extracted from the spleen in rAAV2 encoding IL-12 mice strongly exhibited cytotoxic activity compared to the control groups (p<0.001). The IgG1, IgG2a, and IgM also showed a significant increase in the rAAV2 encoding IL-12 group compared to the control groups (p<0.05). The tumor growth rate decreased obviously in the rAAV2 encoding IL-12 group with a significant difference from the control groups (p<0.001). This study demonstrated an encouraging result of immunomodulative therapy in malignant brain tumors by rAAV2 carrying IL-12 through activating NK cells.
    關聯: INTERNATIONAL JOURNAL OF ONCOLOGY 35(6):1361-1367
    显示于类别:[免疫學研究所] 期刊論文

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