Immunological properties and vaccine efficacy of murine dendritic cells simultaneously expressing melanoma-associated antigen and interleukin-12

被引:0
|
作者
Naoki Okada
Sayaka Iiyama
Yuka Okada
Hiroyuki Mizuguchi
Takao Hayakawa
Shinsaku Nakagawa
Tadanori Mayumi
Takuya Fujita
Akira Yamamoto
机构
[1] Kyoto Pharmaceutical University,Department of Biopharmaceutics
[2] Osaka University,Research Institute for Microbial Diseases
[3] National Institute of Health Sciences,Division of Cellular and Gene Therapy Products
[4] National Institute of Health Sciences,Department of Biopharmaceutics, Graduate School of Pharmaceutical Sciences
[5] Osaka University,undefined
来源
Cancer Gene Therapy | 2005年 / 12卷
关键词
dendritic cell; gene transduction; gp100; IL-12; melanoma;
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学科分类号
摘要
Interleukin (IL)-12 is a key factor for inducing cellular immune responses, which play a central role in the eradication of cancer. In the present study, in order to create a dendritic cell (DC)-based vaccine capable of positively skewing immune response toward a cellular immunity-dominant state, we analyzed immunological characteristics and vaccine efficacy of DCs cotransduced with melanoma-associated antigen (gp100) and IL-12 gene (gp100+IL12/DCs) by using RGD fiber-mutant adenovirus vector (AdRGD), which enables highly efficient gene transduction into DCs. gp100+IL12/DCs could simultaneously express cytoplasmic gp100 and secretory IL-12 at levels comparable to DCs transduced with each gene alone. In comparison with DCs transduced with gp100 alone (gp100/DCs), upregulation of major histocompatibility complex class I, CD40, and CD86 molecules on the cell surface and more potent T-cell-stimulating ability for proliferation and interferon-γ secretion were observed as characteristic changes in gp100+IL12/DCs. In addition, administration of gp100+IL12/DCs, which were prepared by a relatively low dose of AdRGD-IL12, could induce more potent tumor-specific cellular immunity in the murine B16BL6 melanoma model than vaccination with gp100/DCs. However, antitumor effect and B16BL6-specific cytotoxic T-lymphocyte activity in mice vaccinated with gp100+IL12/DCs diminished with increasing AdRGD-IL12 dose during gene transduction, and paralleled the decrease in presentation levels via MHC class I molecules for antigen transduced with another AdRGD. Collectively, our results suggested that optimization of combined vector dose was required for development of a more efficacious DC-based vaccine for cancer immunotherapy, which relied on genetic engineering to simultaneously express tumor-associated antigen and IL-12.
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页码:72 / 83
页数:11
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