首页> 外文会议>2011 international conference on bioinformatics and biomedical technology >Anti-tumor Immunity Induced by Cross-link Complex Alpha-fetoprotein and Glycoprotein 96
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Anti-tumor Immunity Induced by Cross-link Complex Alpha-fetoprotein and Glycoprotein 96

机译:交联复合甲胎蛋白和糖蛋白96诱导的抗肿瘤免疫

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Purposes: To study the ability of gp96 to induce specific CTL response and its protective effect against AFP-producing tumor, a recombinant vaccine alpha-fetoprotein (AFP)-glycoprotein (gp96) complex was constructed. Material/Methods: A recombinant peptide vaccine was constructed by conjugating mouse alpha-fetoprotein to glycoprotein 96. By way of intracutaneous injection, mice were primed and boosted with recombinant vaccine mAFP/gp96, whereas single mAFP or gp96 injection as controls. The ELISPOT and ELISA were used to measure the frequency of cells producing the cytokine IFN-gama in splenocytes and the level of anti-AFP antibody in serum from immunized mice respectively. In vivo tumor challenge was carried out to assess the immune effect of the recombinant vaccine. Results: By recombinant mAFP/gp96 vaccine immunization, the number of splenic cells producing IFN-gama and the level of anti-AFP antibody in serum were significantly higher in mAFP/gp96 group than those in mAFP and gp96 groups (122.50±9.30 IFN-gama spots/106 cells vs 46.40±10.32 IFN-gama spots/106 cells, 12.14±7.33 IFN-gama. spots/106 cells, P<0.01; 164.52± 11.22 ug/mL vs 56.32±8.23 ug/mL, 7.56±3.47 ug/mL, p< 0.01). The tumor volume in mAFP/gp96 group was significantly smaller than that in mAFP and gp96 groups (32.46±6.35 mm3 vs 384.16± 11.43 mm3, 832.54± 12.72 mm3, P< 0.01). Conclusions: The study further confirmed the function of glycoprotein 96's immune adjuvant. Sequential immunization with recombinant mAFP/gp96 vaccine could generate effective specific antitumor immunity on AFP-producing tumor. The recombined mAFP/gp96 vaccine may be suitable for serving as an immunotherapy for hepatocellular carcinoma.
机译:目的:为了研究gp96诱导特异性CTL应答的能力及其对产生AFP的肿瘤的保护作用,构建了重组疫苗甲胎蛋白(AFP)-糖蛋白(gp96)复合物。材料/方法:通过将小鼠甲胎蛋白与糖蛋白96偶联来构建重组肽疫苗。通过皮内注射,小鼠用重组疫苗mAFP / gp96进行初次免疫和加强免疫,而单次mAFP或gp96注射作为对照。用ELISPOT和ELISA分别测量免疫细胞中脾细胞中产生细胞因子IFN-γ的细胞的频率和血清中抗AFP抗体的水平。进行体内肿瘤攻击以评估重组疫苗的免疫效果。结果:通过重组mAFP / gp96疫苗免疫,mAFP / gp96组的血清中产生IFN-γ的脾细胞数量和抗AFP抗体水平明显高于mAFP和gp96组(122.50±9.30 IFN- γ斑点/ 106细胞vs 46.40±10.32IFN-γ斑点/ 106细胞,12.14±7.33IFN-γ斑点/ 106细胞,P <0.01; 164.52±11.22 ug / mL vs 56.32±8.23 ug / mL,7.56±3.47 ug / mL,p <0.01)。 mAFP / gp96组的肿瘤体积明显小于mAFP和gp96组(32.46±6.35 mm3 vs 384.16±11.43 mm3,832.54±12.72 mm3,P <0.01)。结论:该研究进一步证实了糖蛋白96的免疫佐剂的功能。重组mAFP / gp96疫苗的顺序免疫可以对产生AFP的肿瘤产生有效的特异性抗肿瘤免疫。重组的mAFP / gp96疫苗可能适合用作肝细胞癌的免疫疗法。

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