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Examination of influenza specific T cell responses after influenza virus challenge in individuals vaccinated with MVA-NP+M1 vaccine.

机译:在接种MVA-NP + M1疫苗的个体中检测流感病毒后,流感特异性T细胞反应。

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摘要

Current influenza vaccines stimulate neutralising antibody to the haemagglutinin antigen but as there is antigenic drift in HA it is difficult to prepare a vaccine in advance against an emergent strain. A potential strategy is to induce CD8(+) and CD4(+) T cells that recognize epitopes within internal proteins that are less subject to antigenic drift. Augmenting humoral responses to HA with T cell responses to more conserved antigens may result in a more broadly protective vaccine. In this study, we evaluate the quality of influenza specific T cell responses in a clinical trial using MVA-NP+M1 vaccination followed by influenza virus challenge. In vaccinated volunteers, the expression of Granzyme A, Perforin and CD57 on influenza HLA A*02 M158-66 antigen specific cells was higher than non-vaccinated volunteers before and after challenge despite a similar frequency of antigen specific cells. BCL2 expression was lower in vaccinated volunteers. These data indicate that antigen specific T cells are a useful additional measure for use in human vaccination or immunization studies.
机译:当前的流感疫苗刺激针对血凝素抗原的中和抗体,但是由于HA中存在抗原漂移,因此难以预先制备针对紧急菌株的疫苗。潜在的策略是诱导识别内部蛋白质内抗原决定簇的CD8(+)和CD4(+)T细胞,这些抗原较少受抗原漂移的影响。用对更保守的抗原的T细胞应答增强对HA的体液应答可能会产生更广泛的保护性疫苗。在这项研究中,我们在一项使用MVA-NP + M1疫苗接种随后进行流感病毒攻击的临床试验中评估了流感特异性T细胞反应的质量。在接种疫苗的志愿者中,尽管攻击前后抗原抗原细胞的频率相似,但流感病毒HLA A * 02 M158-66抗原特异性细胞上颗粒酶A,穿孔素和CD57的表达要高于未接种疫苗的志愿者。接种疫苗的志愿者中BCL2表达较低。这些数据表明抗原特异性T细胞是用于人类疫苗接种或免疫研究的有用的附加措施。

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