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在禽-人重配疫苗病毒的体外生产过程中以及在人类和灵长类动物体内复制后,对甲型禽流感/野鸭/78病毒减毒的M基因片段和NP基因片段的特性进行研究。

Characterization of the attenuating M and NP gene segments of the avian influenza A/Mallard/78 virus during in vitro production of avian-human reassortant vaccine viruses and after replication in humans and primates.

作者信息

Treanor J J, Tierney E L, London W T, Murphy B R

机构信息

Laboratory of Infectious Disease, National Institute of Allergy and Infectious Diseases, NIH, Bethesda, MD.

出版信息

Vaccine. 1991 Jul;9(7):495-501. doi: 10.1016/0264-410x(91)90035-5.

DOI:10.1016/0264-410x(91)90035-5
PMID:1897305
Abstract

A unique requirement for live attenuated reassortant influenza vaccines is the need to generate new reassortant vaccine viruses with the appearance of each new antigenic variant. Thus, the attenuation phenotype conferred by the attenuated donor influenza virus must remain genetically stable during the generation of each new reassortant vaccine virus. In this study we used nucleotide sequence analysis to evaluate the genetic stability of the attenuating M and NP genes of the avian influenza A/Mallard/NY/6750/78 attenuated donor virus during the in vitro generation and subsequent in vivo replication of avian-human (AH) influenza A reassortant vaccine viruses in monkeys and humans. Nucleotide sequence changes in the M and NP genes occurred at a rate of approximately 0.61 substitutions/1000 nt/reassortant during in vitro generation of four AH reassortant viruses. Only two nucleotide sequence changes occurred in the M and NP gene segments of four isolates of H1N1 or H3N2 AH vaccine viruses following 6-8 days of replication in seronegative children, and neither change affected amino acids previously identified as playing a potential role in attenuation. In addition, there were no changes in the nucleotide sequence of the M and NP genes of single gene AH reassortant viruses following five serial passages in squirrel monkeys. Finally, there was no change in the level or duration of replication of the single gene reassortant viruses in the upper or lower respiratory tract of monkeys following serial passage.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

减毒活重组流感疫苗的一个独特要求是,每当出现新的抗原变异体时,都需要产生新的重组疫苗病毒。因此,减毒供体流感病毒赋予的减毒表型在产生每一种新的重组疫苗病毒的过程中必须保持遗传稳定性。在本研究中,我们使用核苷酸序列分析来评估甲型禽流感A/野鸭/纽约/6750/78减毒供体病毒的减毒M基因和NP基因在禽-人(AH)甲型流感重组疫苗病毒在猴子和人类体内的体外产生及随后的体内复制过程中的遗传稳定性。在四种AH重组病毒的体外产生过程中,M基因和NP基因的核苷酸序列变化速率约为每1000个核苷酸/重组体0.61个替换。在血清阴性儿童中复制6-8天后,H1N1或H3N2 AH疫苗病毒的四个分离株的M基因和NP基因片段仅发生了两个核苷酸序列变化,且这两个变化均未影响先前确定在减毒中起潜在作用的氨基酸。此外,单基因AH重组病毒在松鼠猴中连续传代五次后,M基因和NP基因的核苷酸序列没有变化。最后,连续传代后,单基因重组病毒在猴子上呼吸道或下呼吸道中的复制水平和持续时间没有变化。(摘要截短于250字)

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1
Characterization of the attenuating M and NP gene segments of the avian influenza A/Mallard/78 virus during in vitro production of avian-human reassortant vaccine viruses and after replication in humans and primates.在禽-人重配疫苗病毒的体外生产过程中以及在人类和灵长类动物体内复制后,对甲型禽流感/野鸭/78病毒减毒的M基因片段和NP基因片段的特性进行研究。
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