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Essential sequence of influenza B virus hemagglutinin DNA to provide protection against lethal homologous viral infection.

机译:流感B病毒血凝素DNA的基本序列,以提供致死同源病毒感染的保护。

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摘要

Hemagglutinin (HA) is the main surface glycoprotein of influenza B virus. The B/Ibaraki/2/85 virus HA gene is 1758 bp in length, including signal peptide sequence, HA1 sequence, and HA2 sequence. We previously proved that B/Ibaraki/2/85 HA DNA induced immune response and provided effective protection in mice against challenge with homologous virus. In this study, a series of recombinant plasmids encoding truncated HA gene were constructed by PCR. BALB/c mice were immunized with the plasmids and challenged with a lethal dose of homologous virus. The essential sequence of HA DNA against influenza virus was explored by evaluation of survival rate, lung virus titer, bodyweight change, and serum anti-HA antibody titer of mice. The result showed that serial deletion did not deprive HA DNA of its protective ability until 885 nucleotides (295 amino acids) at 3'-terminal or 9 nucleotides of the signal peptide sequence at 5'-terminal were deleted. When the signal peptide sequence was kept intact and the 5'-terminal deletion started at the beginning of the HA1 sequence, deletion of 51 nucleotides (17 amino acids) made HA DNA lose its protective ability. This suggests that the sequence nt94-876 of B/Ibaraki/2/85 virus HA DNA played an important role in protection against infection.
机译:血凝素(HA)是流感B病毒的主要表面糖蛋白。 B / Ibaraki / 2/85病毒HA基因长度为1758磅,包括信号肽序列,HA1序列和HA2序列。我们之前证明了B / IBARAKI / 2/85 HA DNA诱导免疫应答,并提供了对小鼠的有效保护,以与同源病毒攻击。在该研究中,通过PCR构建编码截短的HA基因的一系列重组质粒。用质粒免疫Balb / c小鼠并用致命剂量的同源病毒攻击。通过评估生存率,肺病毒滴度,体重变化和小鼠的血清抗HA抗体滴度来探讨HA DNA对流感病毒的基本序列。结果表明,连续缺失没有剥夺其保护能力的HA DNA,直至在3'-末端的3'-末端(295个氨基酸)或5'-末端的信号肽序列的9个核苷酸的核苷酸(295个氨基酸)中被删除。当信号肽序列保持完整并且在HA1序列开始时开始5'-末端缺失,51个核苷酸(17个氨基酸)的缺失使HA DNA失去其保护能力。这表明B / Ibaraki / 2/85病毒HA DNA的序列NT94-876在保护免受感染方面发挥了重要作用。

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