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增强痘病毒载体疫苗的免疫原性。

Enhancing poxvirus vectors vaccine immunogenicity.

作者信息

García-Arriaza Juan, Esteban Mariano

机构信息

a Department of Molecular and Cellular Biology; Centro Nacional de Biotecnología; Consejo Superior de Investigaciones Científicas (CSIC); Madrid, Spain.

出版信息

Hum Vaccin Immunother. 2014;10(8):2235-44. doi: 10.4161/hv.28974.

Abstract

Attenuated recombinant poxvirus vectors expressing heterologous antigens from pathogens are currently at various stages in clinical trials with the aim to establish their efficacy. This is because these vectors have shown excellent safety profiles, significant immunogenicity against foreign expressed antigens and are able to induce protective immune responses. In view of the limited efficacy triggered by some poxvirus strains used in clinical trials (i.e, ALVAC in the RV144 phase III clinical trial for HIV), and of the restrictive replication capacity of the highly attenuated vectors like MVA and NYVAC, there is a consensus that further improvements of these vectors should be pursuit. In this review we considered several strategies that are currently being implemented, as well as new approaches, to improve the immunogenicity of the poxvirus vectors. This includes heterologous prime/boost protocols, use of co-stimulatory molecules, deletion of viral immunomodulatory genes still present in the poxvirus genome, enhancing virus promoter strength, enhancing vector replication capacity, optimizing expression of foreign heterologous sequences, and the combined use of adjuvants. An optimized poxvirus vector triggering long-lasting immunity with a high protective efficacy against a selective disease should be sought.

摘要

表达病原体异源抗原的减毒重组痘病毒载体目前正处于临床试验的各个阶段,目的是确定其疗效。这是因为这些载体已显示出优异的安全性、针对外源表达抗原的显著免疫原性,并且能够诱导保护性免疫反应。鉴于临床试验中使用的一些痘病毒株引发的疗效有限(例如,HIV的RV144 III期临床试验中的ALVAC),以及像MVA和NYVAC这样的高度减毒载体的复制能力受限,人们一致认为应该对这些载体进行进一步改进。在本综述中,我们考虑了目前正在实施的几种策略以及新方法,以提高痘病毒载体的免疫原性。这包括异源初免/加强方案、共刺激分子的使用、删除痘病毒基因组中仍然存在的病毒免疫调节基因、增强病毒启动子强度、增强载体复制能力、优化外源异源序列的表达以及佐剂的联合使用。应该寻求一种优化的痘病毒载体,它能引发持久免疫,对特定疾病具有高保护效力。

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