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Influenza nucleoprotein delivered with aluminium salts protects mice from an influenza virus that expresses an altered nucleoprotein sequence

机译:用铝盐递送的流感核蛋白保护小鼠免受表达改变的核蛋白序列的流感病毒的伤害

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摘要

Influenza virus poses a difficult challenge for protective immunity. This virus is adept at altering its surface proteins, the proteins that are the targets of neutralizing antibody. Consequently, each year a new vaccine must be developed to combat the current recirculating strains. A universal influenza vaccine that primes specific memory cells that recognise conserved parts of the virus could prove to be effective against both annual influenza variants and newly emergent potentially pandemic strains. Such a vaccine will have to contain a safe and effective adjuvant that can be used in individuals of all ages. We examine protection from viral challenge in mice vaccinated with the nucleoprotein from the PR8 strain of influenza A, a protein that is highly conserved across viral subtypes. Vaccination with nucleoprotein delivered with a universally used and safe adjuvant, composed of insoluble aluminium salts, provides protection against viruses that either express the same or an altered version of nucleoprotein. This protection correlated with the presence of nucleoprotein specific CD8 T cells in the lungs of infected animals at early time points after infection. In contrast, immunization with NP delivered with alum and the detoxified LPS adjuvant, monophosphoryl lipid A, provided some protection to the homologous viral strain but no protection against infection by influenza expressing a variant nucleoprotein. Together, these data point towards a vaccine solution for all influenza A subtypes.
机译:流感病毒对保护性免疫提出了艰巨的挑战。该病毒擅长改变其表面蛋白,这些蛋白是中和抗体的靶标。因此,每年必须开发一种新疫苗来对抗当前的循环毒株。一种通用的流感疫苗可以启动识别特定病毒的特定存储细胞,从而识别该病毒的保守部分,可以证明对年度流感变种和新近出现的潜在大流行毒株均有效。这种疫苗必须包含可用于所有年龄段的个体的安全有效的佐剂。我们在接种甲型流感病毒PR8株的核蛋白的小鼠中检查了对病毒攻击的保护,该蛋白是跨病毒亚型高度保守的蛋白。用由不溶性铝盐组成的通用且安全的佐剂递送的核蛋白进行疫苗接种,可抵抗表达相同或改变形式的核蛋白的病毒。这种保护与感染后早期时间点感染动物肺中核蛋白特异性CD8 T细胞的存在有关。相反,用明矾和解毒的LPS佐剂单磷酰脂质A递送的NP疫苗对同源病毒株提供了一定的保护,但不能抵抗表达变异核蛋白的流感病毒的感染。这些数据共同指向所有A型流感亚型的疫苗解决方案。

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