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鼻腔免疫接种灭活流感病毒诱导的血凝素特异性抗体的异亚型抗病毒活性。

Heterosubtypic antiviral activity of hemagglutinin-specific antibodies induced by intranasal immunization with inactivated influenza viruses in mice.

机构信息

Division of Global Epidemiology, Research Center for Zoonosis Control, Hokkaido University, Sapporo, Japan.

出版信息

PLoS One. 2013 Aug 16;8(8):e71534. doi: 10.1371/journal.pone.0071534. eCollection 2013.

Abstract

Influenza A virus subtypes are classified on the basis of the antigenicity of their envelope glycoproteins, hemagglutinin (HA; H1-H17) and neuraminidase. Since HA-specific neutralizing antibodies are predominantly specific for a single HA subtype, the contribution of antibodies to the heterosubtypic immunity is not fully understood. In this study, mice were immunized intranasally or subcutaneously with viruses having the H1, H3, H5, H7, H9, or H13 HA subtype, and cross-reactivities of induced IgG and IgA antibodies to recombinant HAs of the H1-H16 subtypes were analyzed. We found that both subcutaneous and intranasal immunizations induced antibody responses to multiple HAs of different subtypes, whereas IgA was not detected remarkably in mice immunized subcutaneously. Using serum, nasal wash, and trachea-lung wash samples of H9 virus-immunized mice, neutralizing activities of cross-reactive antibodies were then evaluated by plaque-reduction assays. As expected, no heterosubtypic neutralizing activity was detected by a standard neutralization test in which viruses were mixed with antibodies prior to inoculation into cultured cells. Interestingly, however, a remarkable reduction of plaque formation and extracellular release of the H12 virus, which was bound by the H9-induced cross-reactive antibodies, was observed when infected cells were subsequently cultured with the samples containing HA-specific cross-reactive IgA. This heterosubtypic plaque reduction was interfered when the samples were pretreated with anti-mouse IgA polyclonal serum. These results suggest that the majority of HA-specific cross-reactive IgG and IgA antibodies produced by immunization do not block cellular entry of viruses, but cross-reactive IgA may have the potential to inhibit viral egress from infected cells and thus to play a role in heterosubtypic immunity against influenza A viruses.

摘要

甲型流感病毒亚型根据其包膜糖蛋白血凝素 (HA; H1-H17) 和神经氨酸酶的抗原性进行分类。由于针对 HA 的特异性中和抗体主要针对单一 HA 亚型,因此抗体对异源型免疫的贡献尚不完全清楚。在这项研究中,通过鼻腔内或皮下免疫 H1、H3、H5、H7、H9 或 H13 HA 亚型的病毒,分析诱导的 IgG 和 IgA 抗体对 H1-H16 亚型重组 HA 的交叉反应性。我们发现皮下和鼻腔内免疫均可诱导针对不同亚型多种 HA 的抗体反应,而皮下免疫的小鼠中 IgA 则未明显检测到。使用 H9 病毒免疫小鼠的血清、鼻腔冲洗液和气管-肺冲洗液样本,然后通过蚀斑减少测定评估交叉反应性抗体的中和活性。不出所料,在标准中和试验中,用病毒与抗体混合后再接种到培养细胞中,未检测到异源型中和活性。然而,有趣的是,当用含有 HA 特异性交叉反应性 IgA 的样本培养感染细胞时,观察到与 H9 诱导的交叉反应性抗体结合的 H12 病毒的蚀斑形成和细胞外释放显著减少。当用抗小鼠 IgA 多克隆血清预处理样本时,这种异源型蚀斑减少被干扰。这些结果表明,免疫产生的大多数 HA 特异性交叉反应性 IgG 和 IgA 抗体不会阻止病毒进入细胞,但交叉反应性 IgA 可能具有抑制感染细胞中病毒释放的潜力,从而在针对甲型流感病毒的异源型免疫中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db13/3745432/e7c1196c0dda/pone.0071534.g001.jpg

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