在患有严重呼吸道感染的婴儿中,呼吸道合胞病毒特异性抗体对自然杀伤细胞的激活作用减弱,且与Fc糖基化相关。
Natural killer cell activation by respiratory syncytial virus-specific antibodies is decreased in infants with severe respiratory infections and correlates with Fc-glycosylation.
作者信息
van Erp Elisabeth A, Lakerveld Anke J, de Graaf Erik, Larsen Mads D, Schepp Rutger M, Hipgrave Ederveen Agnes L, Ahout Inge Ml, de Haan Cornelis Am, Wuhrer Manfred, Luytjes Willem, Ferwerda Gerben, Vidarsson Gestur, van Kasteren Puck B
机构信息
Centre for Infectious Disease Control National Institute for Public Health and the Environment (RIVM) Bilthoven The Netherlands.
Section Pediatric Infectious Diseases Laboratory of Medical Immunology Radboud Institute for Molecular Life Sciences, Radboudumc Nijmegen The Netherlands.
出版信息
Clin Transl Immunology. 2020 Feb 19;9(2):e1112. doi: 10.1002/cti2.1112. eCollection 2020.
OBJECTIVES
Respiratory syncytial virus (RSV) is a major cause of severe lower respiratory tract infections in infants, and there is no vaccine available. In early life, the most important contributors to protection against infectious diseases are the innate immune response and maternal antibodies. However, antibody-mediated protection against RSV disease is incompletely understood, as both antibody levels and neutralisation capacity correlate poorly with protection. Since antibodies also mediate natural killer (NK) cell activation, we investigated whether this functionality correlates with RSV disease.
METHODS
We performed an observational case-control study including infants hospitalised for RSV infection, hernia surgery or RSV-negative respiratory viral infections. We determined RSV antigen-specific antibody levels in plasma using a multiplex immunoassay. Subsequently, we measured the capacity of these antibodies to activate NK cells. Finally, we assessed Fc-glycosylation of the RSV-specific antibodies by mass spectrometry.
RESULTS
We found that RSV-specific maternal antibodies activate NK cells . While concentrations of RSV-specific antibodies did not differ between cases and controls, antibodies from infants hospitalised for severe respiratory infections (RSV and/or other) induced significantly less NK cell interferon-γ production than those from uninfected controls. Furthermore, NK cell activation correlated with Fc-fucosylation of RSV-specific antibodies, but their glycosylation status did not significantly differ between cases and controls.
CONCLUSION
Our results suggest that Fc-dependent antibody function and quality, exemplified by NK cell activation and glycosylation, contribute to protection against severe RSV disease and warrant further studies to evaluate the potential of using these properties to evaluate and improve the efficacy of novel vaccines.
目的
呼吸道合胞病毒(RSV)是婴儿严重下呼吸道感染的主要病因,且尚无可用疫苗。在生命早期,抵御传染病的最重要因素是先天免疫反应和母体抗体。然而,抗体介导的对RSV疾病的保护作用尚未完全明确,因为抗体水平和中和能力与保护作用的相关性都很差。由于抗体也介导自然杀伤(NK)细胞活化,我们研究了这种功能是否与RSV疾病相关。
方法
我们进行了一项观察性病例对照研究,纳入因RSV感染、疝气手术或RSV阴性呼吸道病毒感染而住院的婴儿。我们使用多重免疫测定法测定血浆中RSV抗原特异性抗体水平。随后,我们测量了这些抗体激活NK细胞的能力。最后,我们通过质谱评估RSV特异性抗体的Fc糖基化。
结果
我们发现RSV特异性母体抗体可激活NK细胞。虽然病例组和对照组之间RSV特异性抗体浓度没有差异,但因严重呼吸道感染(RSV和/或其他)住院的婴儿的抗体诱导的NK细胞干扰素-γ产生明显少于未感染对照组。此外,NK细胞活化与RSV特异性抗体的Fc岩藻糖基化相关,但病例组和对照组之间其糖基化状态没有显著差异。
结论
我们的结果表明,以NK细胞活化和糖基化为例的Fc依赖性抗体功能和质量有助于抵御严重RSV疾病,值得进一步研究以评估利用这些特性评估和提高新型疫苗疗效的潜力。
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