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人乳头瘤病毒16型抗原与泛素融合的重组E6E7的表达、多聚泛素化及治疗潜力

Expression, Polyubiquitination, and Therapeutic Potential of Recombinant E6E7 from HPV16 Antigens Fused to Ubiquitin.

作者信息

de Oliveira Liliane M Fernandes, Morale Mirian G, Chaves Agtha A M, Demasi Marilene, Ho Paulo L

机构信息

Laboratório de Biotecnologia Molecular I, Centro de Biotecnologia, Instituto Butantan, Av. Vital Brasil 1500, São Paulo, SP, Brazil.

Laboratório de Bioquímica e Biofísica, Instituto Butantan, Av. Vital Brasil 1500, São Paulo, SP, Brazil.

出版信息

Mol Biotechnol. 2017 Jan;59(1):46-56. doi: 10.1007/s12033-016-9990-6.

Abstract

Ubiquitin-proteasome system plays an essential role in the immune response due to its involvement in the antigen generation and presentation to CD8 T cells. Hereby, ubiquitin fused to antigens has been explored as an immunotherapeutic strategy that requires the activation of cytotoxic T lymphocytes. Here we propose to apply this ubiquitin fusion approach to a recombinant vaccine against human papillomavirus 16-infected cells. E6E7 multi-epitope antigen was fused genetically at its N- or C-terminal end to ubiquitin and expressed in Escherichia coli as inclusion bodies. The antigens were solubilized using urea and purified by nickel affinity chromatography in denatured condition. Fusion of ubiquitin to E6E7 resulted in marked polyubiquitination in vitro mainly when fused to the E6E7 N-terminal. When tested in a therapeutic scenario, the fusion of ubiquitin to E6E7 reinforced the anti-tumor protection and increased the E6/E7-specific cellular immune responses. Present results encourage the investigation of the adjuvant potential of the ubiquitin fusion to recombinant vaccines requiring CD8 T cells.

摘要

泛素-蛋白酶体系统因其参与抗原生成及向CD8 T细胞的呈递而在免疫应答中发挥着至关重要的作用。据此,与抗原融合的泛素已被探索作为一种需要激活细胞毒性T淋巴细胞的免疫治疗策略。在此,我们提议将这种泛素融合方法应用于针对人乳头瘤病毒16感染细胞的重组疫苗。E6E7多表位抗原在其N端或C端与泛素进行基因融合,并作为包涵体在大肠杆菌中表达。抗原用尿素溶解,并在变性条件下通过镍亲和层析进行纯化。泛素与E6E7融合主要在与E6E7 N端融合时在体外导致明显的多聚泛素化。在治疗方案中进行测试时,泛素与E6E7的融合增强了抗肿瘤保护作用,并增加了E6/E7特异性细胞免疫应答。目前的结果鼓励对泛素融合对需要CD8 T细胞的重组疫苗的佐剂潜力进行研究。

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