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使用甲胎蛋白基因的疫苗疗法对小鼠肝细胞癌的多样疗效。

Diverse efficacy of vaccination therapy using the alpha-fetoprotein gene against mouse hepatocellular carcinoma.

作者信息

Saeki Akira, Nakao Kazuhiko, Nagayama Yuji, Yanagi Kenji, Matsumoto Kojiro, Hayashi Toshinobu, Ishikawa Hiroki, Hamasaki Keisuke, Ishii Nobuko, Eguchi Katsumi

机构信息

First Department of Internal Medicine, Nagasaki University Graduate School of Biomedical Sciences, Nagasaki, Japan.

出版信息

Int J Mol Med. 2004 Jan;13(1):111-6.

Abstract

Antitumor vaccination therapy approaches using naked plasmid DNA or recombinant viruses encoding tumor-associated antigens are currently in development. In the present study, we examined the therapeutic efficacy of vaccination using the mouse alpha-fetoprotein (AFP) gene in mouse hepatocellular carcinoma (HCC) cells. C57L/J or C3H/HeN mice were primed with an injection of naked plasmid DNA expressing mouse AFP followed by a booster of replication-defective adenovirus expressing mouse AFP (plasmid-AFP prime/adenovirus-AFP booster vaccination). The mice were then challenged with high AFP-producing Hepa1-6 cells or low AFP-producing MH134 cells, respectively, and the tumor growth rate was monitored. Plasmid-AFP prime/adenovirus-AFP booster vaccination promoted protective immunity against Hepa1-6 cells, and significantly increased the number of interferon-gamma-producing splenic cells in C57L/J mice. In addition, this vaccination protocol repressed the growth of pre-established Hepa1-6 tumors in C57L/J mice. However, plasmid-AFP prime/adenovirus-AFP booster vaccination did not induce protective immunity against MH134 cells in C3H/HeN mice. These results suggest that vaccination with the AFP gene is a promising strategy to treat HCC, but its outcome may be affected by the level of AFP expression in HCC or by the immunological response of the host.

摘要

目前正在研发使用裸质粒DNA或编码肿瘤相关抗原的重组病毒的抗肿瘤疫苗治疗方法。在本研究中,我们检测了使用小鼠甲胎蛋白(AFP)基因对小鼠肝癌(HCC)细胞进行疫苗接种的治疗效果。给C57L/J或C3H/HeN小鼠注射表达小鼠AFP的裸质粒DNA进行初次免疫,随后用表达小鼠AFP的复制缺陷型腺病毒进行加强免疫(质粒-AFP初次免疫/腺病毒-AFP加强免疫接种)。然后分别用高AFP产生的Hepa1-6细胞或低AFP产生的MH134细胞对小鼠进行攻击,并监测肿瘤生长速率。质粒-AFP初次免疫/腺病毒-AFP加强免疫接种促进了对Hepa1-6细胞的保护性免疫,并显著增加了C57L/J小鼠中产生干扰素-γ的脾细胞数量。此外,该接种方案抑制了C57L/J小鼠中预先建立的Hepa1-6肿瘤的生长。然而,质粒-AFP初次免疫/腺病毒-AFP加强免疫接种在C3H/HeN小鼠中未诱导对MH134细胞的保护性免疫。这些结果表明,用AFP基因进行疫苗接种是治疗肝癌的一种有前景的策略,但其结果可能受肝癌中AFP表达水平或宿主免疫反应的影响。

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