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鼻腔内给予重组核蛋白可预防多种甲型流感病毒亚型感染

Protection against multiple influenza A virus subtypes by intranasal administration of recombinant nucleoprotein.

机构信息

Shanghai Institute of Biological Products, China.

出版信息

Arch Virol. 2010 Nov;155(11):1765-75. doi: 10.1007/s00705-010-0756-3. Epub 2010 Jul 22.

Abstract

Vaccination is a cost-effective way to control the influenza epidemic. Vaccines based on highly conserved antigens can provide protection against different influenza A strains and subtypes. In this study, the recombinant nucleoprotein (rNP) of the A/PR/8/34 (H1N1) influenza virus strain was effectively expressed using a prokaryotic expression system and then purified with a nickel-charged Sepharose affinity column as a candidate component for an influenza vaccine. The rNP was administered intranasally three times at 3-week intervals to female BALB/c mice in combination with an adjuvant (cholera toxin B subunit containing 0.2% of the whole toxin). Twenty-one days after the last immunization, the mice were challenged with homologous or heterologous influenza viruses at a lethal dose. The results showed that intranasal immunization of 10 μg rNP with adjuvant completely protected the immunized mice against the homologous influenza virus, and immunization with 100 μg rNP in combination with adjuvant provided good cross-protection against heterologous H5N1 and H9N2 avian influenza viruses. The results indicate that such a vaccine administered intranasally can induce mucosal and cell-mediated immunity, thus having the potential to control epidemics caused by new emerging influenza viruses.

摘要

接种疫苗是控制流感流行的一种具有成本效益的方法。基于高度保守抗原的疫苗可以提供针对不同甲型流感病毒株和亚型的保护。在这项研究中,使用原核表达系统有效地表达了 A/PR/8/34(H1N1)流感病毒株的重组核蛋白(rNP),然后用镍 charged Sepharose 亲和柱纯化,作为流感疫苗的候选成分。rNP 与佐剂(含有 0.2%全毒素的霍乱毒素 B 亚单位)一起通过鼻腔内给药三次,间隔 3 周。最后一次免疫后 21 天,用同源或异源流感病毒以致死剂量对小鼠进行攻毒。结果表明,用佐剂鼻腔内免疫 10 μg rNP 可完全保护免疫小鼠免受同源流感病毒的侵害,而用佐剂联合 100 μg rNP 免疫可对异源 H5N1 和 H9N2 禽流感病毒提供良好的交叉保护作用。这些结果表明,这种经鼻腔内给药的疫苗可以诱导黏膜和细胞介导的免疫,因此具有控制新出现的流感病毒引起的流行的潜力。

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