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Induction of antibody response against hepatitis E virus (HEV) with recombinant human papillomavirus pseudoviruses expressing truncated HEV capsid proteins in mice

机译:表达重组人乳头瘤病毒衣壳蛋白的重组人乳头瘤病毒假病毒诱导对戊型肝炎病毒(HEV)的抗体反应

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A hepatitis E virus (HEV) vaccine Would be Valuable to reduce the morbidity and mortality associated with the infection in endemic areas. HEV pseudocapsids and epidermal delivery of HEV ORF2 DNA vaccine by gene-gun have been shown to confer protection against virus challenge in monkeys. Vectorization of a DNA vaccine by virus-like particles is a new immunization approach. We report here the successful immunization of mice with two ORF2 genes encapsidated into human papillomavirus type 31 virus-like particles. The HEV genes ORF2(112-660) and ORF2(112-608) were optimized for expression in mammalian cells and inserted in a baculovirus-derived vector for expression in insect cells. When expressed in Sf21 insect cells, ORF2(112-660) led to the production of irregular 15 nm particles that accumulated in the cytoplasm of the cells, whereas ORF2(112-608) induced the production of IS nm particles that were present in both the cell culture medium and the cell cytoplasm. Anti-HEV immune responses were higher for the 15 Finn particles (HEV112-660) than that for to the 18 nm particles (HEV112-608). Delivery into mice of two HEV ORF2 genes via a papillomavirus VLP was very effective in the induction of anti-HEV antibodies. In addition, an effective immune response to human papillomavirus capsids occurred. These engineered pseudoviruses were thus demonstrated to induce immune responses to both hepatitis E virus and human papillomavirus when they were administered to mice intramuscularly. (C) 2008 Elsevier Ltd. All Fights reserved.
机译:戊型肝炎病毒(HEV)疫苗对于减少流行地区感染的发病率和死亡率将具有重要意义。 HEV假衣壳和通过基因枪的HEV ORF2 DNA疫苗的表皮递送已显示出对猴子的病毒攻击具有保护作用。通过病毒样颗粒对DNA疫苗进行载体化是一种新的免疫方法。我们在这里报告成功地免疫了衣壳化入人类乳头瘤病毒31型病毒样颗粒的两个ORF2基因。 HEV基因ORF2(112-660)和ORF2(112-608)经过优化,可在哺乳动物细胞中表达,并插入杆状病毒衍生的载体中,可在昆虫细胞中表达。当在Sf21昆虫细胞中表达时,ORF2(112-660)导致产生不规则的15 nm颗粒,这些颗粒积聚在细胞的细胞质中,而ORF2(112-608)诱导了在两种细胞中均存在的IS nm颗粒的产生。细胞培养基和细胞质。 15 Finn颗粒(HEV112-660)的抗HEV免疫反应高于18 nm颗粒(HEV112-608)的抗HEV免疫反应。通过乳头瘤病毒VLP将两个HEV ORF2基因传递给小鼠在诱导抗HEV抗体方面非常有效。另外,发生了对人乳头瘤病毒衣壳的有效免疫反应。因此,当将这些工程伪病毒肌肉注射给小鼠时,可诱导对戊型肝炎病毒和人乳头瘤病毒的免疫反应。 (C)2008 Elsevier Ltd.版权所有。

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