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首页> 美国卫生研究院文献>Journal of Virology >Regression of Established Human Papillomavirus Type 16 (HPV-16) Immortalized Tumors In Vivo by Vaccinia Viruses Expressing Different Forms of HPV-16 E7 Correlates with Enhanced CD8+ T-Cell Responses That Home to the Tumor Site
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Regression of Established Human Papillomavirus Type 16 (HPV-16) Immortalized Tumors In Vivo by Vaccinia Viruses Expressing Different Forms of HPV-16 E7 Correlates with Enhanced CD8+ T-Cell Responses That Home to the Tumor Site

机译:表达不同形式HPV-16 E7的痘苗病毒体内体内已建立的人类乳头瘤病毒16型(HPV-16)永生化肿瘤的消退与肿瘤部位的CD8 + T细胞应答增强相关

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Using vaccinia virus as a live vector, we show that the expression of human papillomavirus type 16 (HPV-16) E7 fused to a nonhemolytic portion of the Listeria monocytogenes virulence factor, listeriolysin O (LLO), induces an immune response that causes the regression of established HPV-16 immortalized tumors in C57BL/6 mice. The vaccinia virus construct expressing LLO fused to E7 (VacLLOE7) was compared with two previously described vaccinia virus constructs: one that expresses unmodified E7 (VacE7) and another that expresses E7 in a form designed to direct it to intracellular lysosomal compartments and improve major histocompatibility complex class II-restricted responses (VacSigE7LAMP-1). C57BL/6 mice bearing established HPV-16 immortalized tumors of 5 or 8 mm were treated with each of these vaccines. Fifty percent of the mice treated with VacLLOE7 remained tumor free 2 months after tumor inoculation, whereas 12 to 25% of the mice were tumor free after treatment with VacSigE7LAMP-1 (depending on the size of the tumor). No mice were tumor free in the group given VacE7. Compared to VacE7, VacSigE7LAMP-1 and VacLLOE7 resulted in increased numbers of H2-Db-specific tetramer-positive CD8+ T cells in mouse spleens that produced gamma interferon and tumor necrosis factor alpha upon stimulation with RAHYNIVTF peptide. In addition, the highest frequency of tetramer-positive T cells was seen in the tumor sites of mice treated with VacLLOE7. An increased efficiency of E7-specific lysis by splenocytes from mice immunized with VacLLOE7 was also observed. These results indicate that the fusion of E7 with LLO not only enhances antitumor therapy by improving the tumoricidal function of E7-specific CD8+ T cells but may also increase the number of antigen-specific CD8+ T cells in the tumor, the principle site of antigen expression.
机译:使用牛痘病毒作为活载体,我们显示与单核细胞增生李斯特菌毒力因子李斯特菌溶血素O(LLO)的非溶血性部分融合的人乳头瘤病毒16型(HPV-16)E7的表达诱导了引起退化的免疫反应C57BL / 6小鼠中已建立的HPV-16永生肿瘤。将表达与E7融合的LLO的痘苗病毒构建体(VacLLOE7)与先前描述的两种痘苗病毒构建体进行了比较:一种表达未修饰的E7(VacE7),另一种表达E7的形式旨在将其引导至细胞内溶酶体区室并改善主要组织相容性复杂的II类限制响应(VacSigE7LAMP-1)。用这些疫苗中的每一种治疗带有5或8毫米HPV-16永生化肿瘤的C57BL / 6小鼠。在接种肿瘤后2个月,接受VacLLOE7治疗的小鼠中有50%保持无肿瘤,而接受VacSigE7LAMP-1治疗的小鼠中有12至25%没有肿瘤(取决于肿瘤的大小)。在给予VacE7的组中,没有小鼠没有肿瘤。与VacE7相比,VacSigE7LAMP-1和VacLLOE7导致小鼠脾脏中H2-D b 特异性四聚体阳性CD8 + T细胞数量增加,产生γ干扰素和肿瘤。 RAHYNIVTF肽刺激后坏死因子α。另外,在用VacLLOE7治疗的小鼠的肿瘤部位中,发现四聚体阳性T细胞的频率最高。还观察到用VacLLOE7免疫的小鼠脾细胞对E7特异性裂解的效率提高。这些结果表明,E7与LLO的融合不仅可以通过改善E7特异性CD8 + T细胞的杀伤功能来增强抗肿瘤治疗,而且还可以增加抗原特异性CD8 +的数量。 T细胞是肿瘤中抗原表达的主要部位。

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