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一种细菌表达的戊型肝炎颗粒疫苗:对灵长类动物的抗原性、免疫原性和保护性。

A bacterially expressed particulate hepatitis E vaccine: antigenicity, immunogenicity and protectivity on primates.

作者信息

Li Shao W, Zhang Jun, Li Yi M, Ou Shan H, Huang Guo Y, He Zhi Q, Ge Sheng X, Xian Yang L, Pang Shu Q, Ng Mun H, Xia Ning S

机构信息

The Key Laboratory of the Ministry of Education for Cell Biology and Tumor Cell Engineering, School of Life Sciences, Xiamen University, Xiamen 361005, China.

出版信息

Vaccine. 2005 Apr 22;23(22):2893-901. doi: 10.1016/j.vaccine.2004.11.064.

Abstract

It was evaluated its antigenicity, immunogenicity and efficacy of a candidate recombinant hepatitis E virus (HEV) vaccine, referred hitherto as HEV 239 vaccine. The vaccine peptide has a 26 amino acids extension from the N terminal of another peptide, E2, of the HEV capsid protein, which has been shown to protect monkeys against HEV infection previously. The vaccine peptide is similar as E2 in that: first, the vaccine peptide migrates predominantly as dimer in SDS-PAGE and it is dissociated into monomers by heating; second, its dimeric form of which predominantly recognized by HEV reactive human serum; and third, it shows the same pattern of reaction as E2 with a panel of eight monoclonal antibodies that had been raised against E2. In contrast to E2, the vaccine peptide aggregates to form particles of 13 nm mean radius, and consequently, it is more than 240 times more immunogenic than E2. Using alum as adjuvant, immunizing dose determined in mice was 80-250 ng for the vaccine and >60 microg for E2. Rhesus monkeys twice vaccinated with a 10 microg or a 20 microg formulation of this vaccine showed essentially the same antibody response, whereas the response to a 5 microg formulation was delayed but reached similar antibody levels. All the three vaccine formulations afford complete protection against infection with 10(4) genome equivalent dose of the homologous genotype 1 virus. At higher virus dose of 10(7), the same vaccine formulation partially protected against the infection and completely protected against hepatitis. The efficacy of the vaccine was essentially the same for the homologous genotype 1 virus and heterologous genotype 4 virus.

摘要

对一种候选重组戊型肝炎病毒(HEV)疫苗(迄今称为HEV 239疫苗)的抗原性、免疫原性和效力进行了评估。该疫苗肽在HEV衣壳蛋白的另一种肽E2的N端有26个氨基酸的延伸,此前已证明E2能保护猴子免受HEV感染。该疫苗肽与E2相似之处在于:第一,该疫苗肽在SDS-PAGE中主要以二聚体形式迁移,加热后解离为单体;第二,其主要被HEV反应性人血清识别的二聚体形式;第三,它与一组针对E2产生的八种单克隆抗体的反应模式与E2相同。与E2不同的是,该疫苗肽聚集形成平均半径为13nm的颗粒,因此,其免疫原性比E2高240倍以上。以明矾作为佐剂,在小鼠中确定的该疫苗免疫剂量为80-250ng,而E2的免疫剂量>60μg。用10μg或20μg该疫苗制剂对恒河猴进行两次接种,显示出基本相同的抗体反应,而对5μg制剂的反应延迟,但达到了相似的抗体水平。所有这三种疫苗制剂对10⁴基因组等效剂量的同源1型病毒感染均提供完全保护。在10⁷的更高病毒剂量下,相同的疫苗制剂对感染有部分保护作用,对肝炎有完全保护作用。该疫苗对同源1型病毒和异源4型病毒的效力基本相同。

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