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Developing a platform system for gene delivery: amplifying virus-like particles (AVLP) as an influenza vaccine

机译:开发用于基因传递的平台系统:扩增病毒样颗粒(AVLP)作为流感疫苗

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摘要

Delivery of a gene of interest to target cells is highly desirable for translational medicine, such as gene therapy, regenerative medicine, vaccine development, and studies of gene function. Parainfluenza virus 5 (PIV5), a paramyxovirus with a negative-sense RNA genome, normally infects cells without causing obvious cytopathic effect, and it can infect many cell types. To exploit these features of PIV5, we established a system generating self-amplifying, virus-like particles (AVLP). Using enhanced green fluorescent protein (EGFP) as a reporter, AVLP encoding EGFP (AVLP–EGFP) successfully delivered and expressed the EGFP gene in primary human cells, including stem cells, airway epithelial cells, monocytes, and T cells. To demonstrate the application of this system for vaccine development, we generated AVLPs to express the HA and M1 antigens from the influenza A virus strain H5N1 (AVLP–H5 and AVLP–M1H5). Immunization of mice with AVLP–H5 and AVLP–M1H5 generated robust antibody and cellular immune responses. Vaccination with a single dose of AVLP–H5 and M1H5 completely protected mice against lethal H5N1 challenge, suggesting that the AVLP-based system is a promising platform for delivery of desirable genes.
机译:对于转化医学,例如基因疗法,再生医学,疫苗开发和基因功能的研究,非常需要将目的基因递送至靶细胞。副流感病毒5(PIV5)是具有负义RNA基因组的副粘病毒,通常感染细胞而不会引起明显的细胞病变作用,并且可以感染许多细胞类型。为了利用PIV5的这些功能,我们建立了一个生成自扩增病毒样颗粒(AVLP)的系统。使用增强型绿色荧光蛋白(EGFP)作为报告基因,编码EGFP(AVLP–EGFP)的AVLP成功地在原代人细胞中传递并表达了EGFP基因,包括干细胞,气道上皮细胞,单核细胞和T细胞。为了证明该系统在疫苗开发中的应用,我们生成了AVLP以表达来自甲型流感病毒H5N1的HA和M1抗原(AVLP–H5和AVLP–M1H5)。用AVLP-H5和AVLP-M1H5免疫小鼠会产生强大的抗体和细胞免疫应答。单剂量的AVLP–H5和M1H5疫苗接种可完全保护小鼠免受致命的H5N1攻击,这表明基于AVLP的系统是提供理想基因的有前途的平台。

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