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Bioengineering a highly productive vaccine strain in embryonated chicken eggs and mammals from a non-pathogenic Glade 2.3.4.4 H5N8 strain

机译:生物工程在非致病林林植物中的胚胎鸡蛋和哺乳动物中的高效疫苗菌株2.3.4.4 H5N8菌株

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摘要

The Glade 2.3.4.4 H5Nx is a highly pathogenic avian influenza (HPAI) virus, which first appeared in China and has spread worldwide since then, including Korea. It is divided into subclades a - d, but the PR8-derived recombinant Glade 2.3.4.4 a viruses replicate inefficiently in embryonated chicken eggs (ECEs). High virus titer in ECEs and no mammalian pathogenicity are the most important prerequisites of efficacious and safer vaccine strains against HPAI. In this study, we have synthesized hemagglutinin (HA) and neuraminidase (NA) genes based on the consensus amino acid sequences of the Glade 2.3.4.4a and b H5N8 HPAIVs, using the GISAID database. We generated PR8-derived H5N8 recombinant viruses with single point mutations in HA and NA, which are related to efficient replication in ECEs. The H103Y mutation in HA increased mammalian pathogenicity as well as virus titer in ECEs, by 10-fold. We also successfully eradicated mammalian pathogenicity in H103Y-bearing H5N8 recombinant virus by exchanging PB2 genes of PR8 and 01310 (Korean H9N2 vaccine strain). The final optimized H5N8 vaccine strain completely protected against a heterologous Glade 2.344c H5N6 HPAIV in chickens, and induced hemagglutination inhibition (HI) antibody in ducks. However, the antibody titer of ducks showed age-dependent results. Thus, H103Y and 01310PB2 gene have been successfully applied to generate a highly productive, safe, and efficacious Glade 2.344 H5N8 vaccine strain in ECEs. (C) 2019 Published by Elsevier Ltd.
机译:林间空地2.3.4.4 H5Nx是高致病性禽流感(HPAI)病毒,它第一次出现在中国,从那时起蔓延全球,其中包括韩国。它分为亚类型A - d,但PR8来源的重组沼地2.3.4.4一个病毒在鸡胚卵(的ECE)低效复制。在欧洲经委会的高病毒滴度,并没有哺乳动物的致病性是对高致病性禽流感的有效和安全的疫苗株的最重要的先决条件。在这项研究中,我们已经合成了血凝素(HA),以及基于所述氨基林地2.3.4.4a的和b H5N8 HPAIVs酸序列,使用全球共享禽流感数据倡议组织数据库的共有神经氨酸酶(NA)基因。我们生成PR8衍生H5N8与HA和NA单点突变,其在的ECE有关有效复制重组病毒。在HA的H103Y突变的ECE增加哺乳动物致病性以及病毒滴度,通过10倍。我们还成功地通过交换PR8和01310(韩国H9N2疫苗株)的PB2基因铲除H103Y轴承H5N8重组病毒的致病性哺乳动物。最终的优化H5N8疫苗株不受异源沼地2.344c H5N6 HPAIV在鸡完全受到保护,并在鸭诱导血细胞凝集抑制(HI)抗体。然而,鸭的抗体滴度呈年龄依赖性的结果。因此,H103Y和01310PB2基因已被成功地应用到产生的ECE高生产力,安全和有效的沼地2.344 H5N8疫苗株。 (c)2019年由elestvier有限公司发布

著录项

  • 来源
    《Vaccine》 |2019年第42期|共8页
  • 作者单位

    Seoul Natl Univ Coll Vet Med Lab Avian Dis Seoul 08826 South Korea;

    Emory Univ Dept Microbiol &

    Immunol Sch Med 1510 Clifton Rd Atlanta GA 30322 USA;

    Seoul Natl Univ Coll Vet Med Lab Avian Dis Seoul 08826 South Korea;

    Anim &

    Plant Quarantine Agcy Avian Dis Div 177 Hyeoksin 8 Ro Gyeongsangbuk Do 39660 South Korea;

    Anim &

    Plant Quarantine Agcy Avian Dis Div 177 Hyeoksin 8 Ro Gyeongsangbuk Do 39660 South Korea;

    Konkuk Univ Coll Vet Med Lab Avian Dis Seoul 05029 South Korea;

    Konkuk Univ Coll Vet Med Lab Avian Dis Seoul 05029 South Korea;

    Konkuk Univ Coll Vet Med Lab Avian Dis Seoul 05029 South Korea;

    Seoul Natl Univ Coll Vet Med Lab Avian Dis Seoul 08826 South Korea;

    Seoul Natl Univ Coll Vet Med Dept Farm Anim Med Lab Poultry Med Seoul 08826 South Korea;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学免疫学;
  • 关键词

    Highly pathogenic avian influenza; Clade 2.3.4.4; H5N8; H103Y; Vaccine;

    机译:高致病性禽流感;Clade 2.3.4.4;H5N8;H103Y;疫苗;

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