首页> 外文期刊>The Journal of Infectious Diseases >Recombinant influenza A virus vaccines for the pathogenic human A/Hong Kong/97 (H5N1) viruses.
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Recombinant influenza A virus vaccines for the pathogenic human A/Hong Kong/97 (H5N1) viruses.

机译:用于致病性人A /香港/ 97(H5N1)病毒的重组甲型流感病毒疫苗。

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Recombinant reassortment technology was used to prepare H5N1 influenza vaccine strains containing a modified hemagglutinin (HA) gene and neuraminidase gene from the A/Hong Kong/156/97 and A/Hong Kong/483/97 isolates and the internal genes from the attenuated cold-adapted A/Ann Arbor/6/60 influenza virus strain. The HA cleavage site (HA1/HA2) of each H5N1 isolate was modified to resemble that of "low-pathogenic" avian strains. Five of 6 basic amino acids at the cleavage site were deleted, and a threonine was added upstream of the remaining arginine. The H5 HA cleavage site modification resulted in the expected trypsin-dependent phenotype without altering the antigenic character of the H5 HA molecule. The temperature-sensitive and cold-adapted phenotype of the attenuated parent virus was maintained in the recombinant strains, and they grew to 108.5-9.4 EID50/mL in eggs. Both H5N1 vaccine virus strains were safe and immunogenic in ferrets and protected chickens against wild-type H5N1 virus challenge.
机译:重组重配技术用于制备H5N1流感疫苗株,该株包含来自A / Hong Kong / 156/97和A / Hong Kong / 483/97分离株的修饰的血凝素(HA)基因和神经氨酸酶基因以及来自减毒感冒的内部基因适应的A / Ann Arbor / 6/60流感病毒株。每个H5N1分离株的HA切割位点(HA1 / HA2)进行了修饰,使其类似于“低致病性”禽流感病毒株。切割位点的6个碱性氨基酸中有5个被删除,苏氨酸在剩余的精氨酸上游添加。 H5 HA切割位点修饰导致预期的胰蛋白酶依赖性表型,而不会改变H5 HA分子的抗原特性。减毒亲本病毒的温度敏感性和冷适应表型在重组菌株中得以维持,它们在卵中生长至108.5-9.4 EID50 / mL。两种H5N1疫苗病毒株均在雪貂中具有安全性和免疫原性,并能保护鸡免受野生型H5N1病毒攻击。

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