首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Viable adenovirus vaccine prototypes: High-level production of a papillomavirus capsid antigen from the major late transcriptional unit
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Viable adenovirus vaccine prototypes: High-level production of a papillomavirus capsid antigen from the major late transcriptional unit

机译:可行的腺病毒疫苗原型:主要晚期转录单位大量生产乳头瘤病毒衣壳抗原

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摘要

Safe, effective, orally delivered, live adenovirus vaccines have been in use for three decades. Recombinant derivatives of the live adenovirus vaccines may prove an economical alternative to current vaccines for a variety of diseases. To explore that possibility, we constructed a series of recombinants that express the major capsid protein (L1) of canine oral papillomavirus (COPV), a model for mucosal human papillomavirus (HPV) infection. Vaccination with virus-like particles (VLPs) composed of recombinant HPV L1 completely prevents persistent HPV infection [Koutsky, L. A., Ault, K. A., Wheeler, C. M., Brown, D. R., Barr, E., Alvarez, F. B., Chiacchierini, L. M. & Jansen, K. U. (2002) N. Engl. J. Med. 347, 1645–1651], suggesting that L1 expressed from recombinant adenoviruses might provide protective immunity. In our recombinants, COPV L1 is incorporated into adenovirus late region 5 (Ad L5) and is expressed as a member of the adenoviral major late transcriptional unit (MLTU). COPV L1 production by the most prolific recombinant is comparable to that of the most abundant adenoviral protein, hexon. COPV L1 production by recombinants is influenced by Ad L5 gene order, the specific mRNA processing signals associated with COPV L1, and the state of a putative splicing inhibitor in the COPV L1 gene. Recombinant COPV L1 protein assembles into VLPs that react with an antibody specific for conformational epitopes on native COPV L1 protein that correlate with protection in vivo. The designs of these recombinants can be applied directly to the production of recombinants appropriate for assessing immunogenicity and protective efficacy in animal models and in human trials.
机译:安全,有效,口服递送的活腺病毒疫苗已经使用了三十年。活性腺病毒疫苗的重组衍生物可能被证明是针对多种疾病的当前疫苗的经济替代。为了探索这种可能性,我们构建了一系列表达犬口腔乳头瘤病毒(COPV)的主要衣壳蛋白(L1)的重组体,这是粘膜人乳头瘤病毒(HPV)感染的模型。用重组HPV L1组成的病毒样颗粒(VLP)进行疫苗接种可完全预防持久性HPV感染[Koutsky,LA,Ault,KA,Wheeler,CM,Brown,DR,Barr,E.,Alvarez,FB,Chiacchierini,LM和Jansen ,KU(2002)N. Engl。 J. Med。 347,1645–1651],表明重组腺病毒表达的L1可能提供保护性免疫。在我们的重组体中,将COPV L1掺入腺病毒晚期区域5(Ad L5)中,并表达为腺病毒主要晚期转录单位(MLTU)的成员。最丰富的重组体产生的COPV L1与最丰富的腺病毒蛋白六邻体相当。重组体产生的COPV L1受Ad L5基因顺序,与COPV L1相关的特定mRNA处理信号以及COPV L1基因中假定的剪接抑制剂状态的影响。重组COPV L1蛋白组装成VLP,这些VLP与对天然COPV L1蛋白的构象表位具有特异性的抗体反应,该抗体与体内保护相关。这些重组体的设计可直接用于生产适合评估动物模型和人体试验的免疫原性和保护功效的重组体。

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