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灭活全流感病毒颗粒疫苗的有效启动作用与病毒 RNA 被抗原呈递细胞摄取有关。

Potent priming by inactivated whole influenza virus particle vaccines is linked to viral RNA uptake into antigen presenting cells.

机构信息

International Institute for Zoonosis Control, Hokkaido University, Sapporo, Japan; International Collaboration Unit, International Institute for Zoonosis Control, Hokkaido University, Sapporo, Japan.

International Institute for Zoonosis Control, Hokkaido University, Sapporo, Japan.

出版信息

Vaccine. 2021 Jun 29;39(29):3940-3951. doi: 10.1016/j.vaccine.2021.05.065. Epub 2021 Jun 2.

Abstract

Current detergent or ether-disrupted split vaccines (SVs) for influenza do not always induce adequate immune responses, especially in young children. This contrasts with the whole virus particle vaccines (WPVs) originally used against influenza that were immunogenic in both adults and children but were replaced by SV in the 1970s due to concerns with reactogenicity. In this study, we re-evaluated the immunogenicity of WPV and SV, prepared from the same batch of purified influenza virus, in cynomolgus macaques and confirmed that WPV is superior to SV in priming potency. In addition, we compared the ability of WPV and SV to induce innate immune responses, including the maturation of dendritic cells (DCs) in vitro. WPV stimulated greater production of inflammatory cytokines and type-I interferon in immune cells from mice and macaques compared to SV. Since these innate responses are likely triggered by the activation of pattern recognition receptors (PRRs) by viral RNA, the quantity and quality of viral RNA in each vaccine were assessed. Although the quantity of viral RNA was similar in the two vaccines, the amount of viral RNA of a length that can be recognized by PRRs was over 100-fold greater in WPV than in SV. More importantly, 1000-fold more viral RNA was delivered to DCs by WPV than by SV when exposed to preparations containing the same amount of HA protein. Furthermore, WPV induced up-regulation of the DC maturation marker CD86 on murine DCs, while SV did not. The present results suggest that the activation of antigen-presenting DCs, by PRR-recognizable viral RNA contained in WPV is responsible for the effective priming potency of WPV observed in naïve mice and macaques. WPV is thus recommended as an alternative option for seasonal influenza vaccines, especially for children.

摘要

当前的洗涤剂或乙醚破裂疫苗(SV)流感并不总是诱导足够的免疫反应,尤其是在幼儿中。这与最初用于流感的全病毒颗粒疫苗(WPV)形成对比,WPV 在成人和儿童中均具有免疫原性,但由于对反应原性的担忧,它在 20 世纪 70 年代被 SV 取代。在这项研究中,我们重新评估了从同一批纯化流感病毒制备的 WPV 和 SV 在食蟹猴中的免疫原性,并证实 WPV 在引发效力方面优于 SV。此外,我们比较了 WPV 和 SV 在诱导先天免疫反应方面的能力,包括体外树突状细胞(DC)的成熟。与 SV 相比,WPV 刺激来自小鼠和食蟹猴的免疫细胞产生更多的炎症细胞因子和 I 型干扰素。由于这些先天反应可能是由病毒 RNA 激活模式识别受体(PRR)引起的,因此评估了每种疫苗中病毒 RNA 的数量和质量。尽管两种疫苗中的病毒 RNA 数量相似,但可被 PRR 识别的病毒 RNA 长度的数量在 WPV 中比在 SV 中多 100 多倍。更重要的是,当暴露于含有相同 HA 蛋白量的制剂时,WPV 向 DC 传递的病毒 RNA 量比 SV 多 1000 倍。此外,WPV 诱导了小鼠 DC 上 DC 成熟标志物 CD86 的上调,而 SV 则没有。目前的结果表明,WPV 中包含的可被 PRR 识别的病毒 RNA 激活抗原呈递 DC,是 WPV 在未致敏小鼠和食蟹猴中观察到的有效引发效力的原因。因此,WPV 被推荐作为季节性流感疫苗的替代选择,尤其是对儿童。

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