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异源两剂埃博拉疫苗接种后的持久自然杀伤细胞反应。

Durable natural killer cell responses after heterologous two-dose Ebola vaccination.

作者信息

Wagstaffe Helen R, Susannini Giada, Thiébaut Rodolphe, Richert Laura, Lévy Yves, Bockstal Viki, Stoop Jeroen N, Luhn Kerstin, Douoguih Macaya, Riley Eleanor M, Lacabaratz Christine, Goodier Martin R

机构信息

Department of Infection Biology, London School of Hygiene and Tropical Medicine, London, UK.

Immunobiology Section, UCL Great Ormond Street Institute of Child Health, London, UK.

出版信息

NPJ Vaccines. 2021 Jan 29;6(1):19. doi: 10.1038/s41541-021-00280-0.

Abstract

Natural killer (NK) cells are implicated among immune effectors after vaccination against viral pathogens, including Ebola virus. The two-dose heterologous Ebola virus vaccine regimen, adenovirus type 26.ZEBOV followed by modified vaccinia Ankara-BN-Filo (EBOVAC2 consortium, EU Innovative Medicines Initiative), induces NK cell activation and anti-Ebola glycoprotein (GP) antibody-dependent NK cell activation post-dose 1, which is further elevated post-dose 2. Here, in a multicentre, phase 2 clinical trial (EBL2001), we demonstrate durable ex vivo NK cell activation 180 days after dose 2, with responses enriched in CD56 NK cells. In vitro antibody-dependent responses to immobilised Ebola GP increased after dose 1, and remained elevated compared to pre-vaccination levels in serum collected 180 days later. Peak NK cell responses were observed post-dose 2 and NK cell IFN-γ responses remained significantly elevated at 180 days post-dose 2. Individual variation in NK cell responses were influenced by both anti-Ebola GP antibody concentrations and intrinsic interindividual differences in NK cell functional capacity. In summary, this study demonstrates durable NK cell responses after Ad26.ZEBOV, MVA-BN-Filo Ebola virus vaccination and could inform the immunological evaluation of future iterations of the vaccine regimen and vaccination schedules.

摘要

在针对包括埃博拉病毒在内的病毒病原体进行疫苗接种后,自然杀伤(NK)细胞被认为是免疫效应器之一。两剂异源埃博拉病毒疫苗方案,即26型腺病毒载体埃博拉疫苗(Ad26.ZEBOV)后接安卡拉痘苗病毒修饰株BN-Filo(EBOVAC2联盟,欧盟创新药物计划),在第1剂接种后可诱导NK细胞活化以及抗埃博拉糖蛋白(GP)抗体依赖性NK细胞活化,在第2剂接种后进一步升高。在此,在一项多中心2期临床试验(EBL2001)中,我们证明在第2剂接种后180天,离体NK细胞活化持久,且CD56 NK细胞中的反应更为富集。在第1剂接种后,对固定化埃博拉GP的体外抗体依赖性反应增加,并且与180天后收集的血清中接种前水平相比仍保持升高。在第2剂接种后观察到NK细胞反应峰值,并且在第2剂接种后180天,NK细胞干扰素-γ反应仍显著升高。NK细胞反应的个体差异受抗埃博拉GP抗体浓度和NK细胞功能能力的个体内在差异影响。总之,本研究证明了Ad26.ZEBOV、MVA-BN-Filo埃博拉病毒疫苗接种后NK细胞反应持久,可为未来疫苗方案和接种计划迭代的免疫学评估提供参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b68/7846750/985c5dce8022/41541_2021_280_Fig1_HTML.jpg

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