Evaluation of novel Epstein-Barr virus-derived antigen formulations for monitoring virus-specific T cells in pediatric patients with infectious mononucleosis.

IF 4 3区医学 Q2 VIROLOGY Virology Journal Pub Date : 2024-06-14 DOI:10.1186/s12985-024-02411-0

Franziska Fischer, Johannes Mücke, Louisa Werny, Katrin Gerrer, Lorenz Mihatsch, Stefanie Zehetmaier, Isa Riedel, Jonas Geisperger, Maren Bodenhausen, Lina Schulte-Hillen, Dieter Hoffmann, Ulrike Protzer, Josef Mautner, Uta Behrends, Tanja Bauer, Nina Körber

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Abstract

Background: Infection with the Epstein-Barr virus (EBV) elicits a complex T-cell response against a broad range of viral proteins. Hence, identifying potential differences in the cellular immune response of patients with different EBV-associated diseases or different courses of the same disorder requires interrogation of a maximum number of EBV antigens. Here, we tested three novel EBV-derived antigen formulations for their ability to reactivate virus-specific T cells ex vivo in patients with EBV-associated infectious mononucleosis (IM).

Methods: We comparatively analyzed EBV-specific CD4+ and CD8+ T-cell responses to three EBV-derived antigen formulations in 20 pediatric patients during the early phase of IM: T-activated EBV proteins (BZLF1, EBNA3A) and EBV-like particles (EB-VLP), both able to induce CD4+ and CD8+ T-cell responses ex vivo, as well as an EBV-derived peptide pool (PP) covering 94 well-characterized CD8+ T-cell epitopes. We assessed the specificity, magnitude, kinetics, and functional characteristics of EBV-specific immune responses at two sequential time points (v1 and v2) within the first six weeks after IM symptom onset (T_onset).

Results: All three tested EBV-derived antigen formulations enabled the detection of EBV-reactive T cells during the early phase of IM without prior T-cell expansion in vitro. EBV-reactive CD4+ and CD8+ T cells were mainly mono-functional (CD4+: mean 64.92%, range 56.15-71.71%; CD8+: mean 58.55%, range 11.79-85.22%) within the first two weeks after symptom onset (v1) with IFN-γ and TNF-secreting cells representing the majority of mono-functional EBV-reactive T cells. By contrast, PP-reactive CD8+ T cells were primarily bi-functional (>60% at v1 and v2), produced IFN-γ and TNF and had more tri-functional than mono-functional components. We observed a moderate correlation between viral load and EBNA3A, EB-VLP, and PP-reactive CD8+ T cells (r_s = 0.345, 0.418, and 0.356, respectively) within the first two weeks after T_onset, but no correlation with the number of detectable EBV-reactive CD4+ T cells.

Conclusions: All three EBV-derived antigen formulations represent innovative and generic recall antigens suitable for monitoring EBV-specific T-cell responses ex vivo. Their combined use facilitates a thorough analysis of EBV-specific T-cell immunity and allows the identification of functional T-cell signatures linked to disease development and severity.

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评估用于监测传染性单核细胞增多症儿科患者病毒特异性 T 细胞的新型 Epstein-Barr 病毒衍生抗原制剂。

背景：感染爱泼斯坦-巴尔病毒（EBV）后，T细胞会对多种病毒蛋白产生复杂的反应。因此，要确定不同 EBV 相关疾病患者或同一疾病不同病程患者细胞免疫反应的潜在差异，就需要检测尽可能多的 EBV 抗原。在此，我们测试了三种新型 EBV 衍生抗原制剂在 EBV 相关传染性单核细胞增多症（IM）患者体内活化病毒特异性 T 细胞的能力：我们比较分析了20名儿童患者在感染性单核细胞增多症早期对三种EBV衍生抗原制剂的EBV特异性CD4+和CD8+T细胞反应：T激活的EBV蛋白（BZLF1、EBNA3A）和EBV样颗粒（EB-VLP）都能诱导体内CD4+和CD8+T细胞应答，EBV衍生的多肽池（PP）涵盖了94个特征明确的CD8+T细胞表位。我们评估了 IM 症状发作（Tonset）后六周内两个连续时间点（v1 和 v2）上 EBV 特异性免疫反应的特异性、程度、动力学和功能特征：结果：所有三种测试的EBV衍生抗原制剂都能在IM早期阶段检测到EBV反应性T细胞，而无需事先在体外进行T细胞扩增。EBV反应性CD4+和CD8+T细胞主要是单功能的（CD4+：平均64.92%，范围56.15-71.71%；CD8+：平均58.55%，范围11.79-85.22%），其中分泌IFN-γ和TNF的细胞占单功能EBV反应性T细胞的大多数。相比之下，对 PP 有反应的 CD8+ T 细胞主要是双功能细胞（在 v1 和 v2 期均大于 60%），能分泌 IFN-γ 和 TNF，三功能成分多于单功能成分。我们观察到，在Tonset后的头两周内，病毒载量与EBNA3A、EB-VLP和PP反应性CD8+T细胞之间存在中度相关性（rs分别为0.345、0.418和0.356），但与可检测到的EBV反应性CD4+T细胞数量没有相关性：所有这三种EBV衍生抗原制剂都是创新的通用召回抗原，适合用于监测体内外EBV特异性T细胞反应。它们的联合使用有助于对 EBV 特异性 T 细胞免疫进行全面分析，并能识别与疾病发展和严重程度相关的功能性 T 细胞特征。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Virology Journal 医学-病毒学

CiteScore

7.40

自引率

2.10%

发文量

186

审稿时长

1 months

期刊介绍： Virology Journal is an open access, peer reviewed journal that considers articles on all aspects of virology, including research on the viruses of animals, plants and microbes. The journal welcomes basic research as well as pre-clinical and clinical studies of novel diagnostic tools, vaccines and anti-viral therapies. The Editorial policy of Virology Journal is to publish all research which is assessed by peer reviewers to be a coherent and sound addition to the scientific literature, and puts less emphasis on interest levels or perceived impact.