流感病毒感染过程中新生儿 CD8+ T 细胞免疫优势层次的改变对多肽疫苗接种的影响

Viruses Pub Date : 2024-08-09 DOI:10.3390/v16081271
Luke Heil, Samantha Jewell, J. Lines, Beth A. Garvy
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摘要

与成人相比,新生儿更容易感染流感病毒,导致发病率和死亡率增加,病毒清除延迟。产生有效的 CD8+ T 细胞反应对于改善易感人群的疫苗接种效果可能很重要,但新生儿 T 细胞的反应往往与成人细胞不同。我们试图了解新生儿感染流感期间 CD8+ T 细胞的特异性和免疫优势,以及与成人层次结构的差异会如何影响多肽疫苗的效果。新生 C57BL/6 小鼠在流感感染期间显示出改变的 CD8+ T 细胞免疫优势等级,优先对流感蛋白 PA 中的一个表位做出反应,而不是成人对 NP 和 PA 的共同优势反应。与成年小鼠首次感染相比,幼鼠首次感染时的异亚型感染也显示出免疫优势的改变和保护能力的降低。通过收养性转移感染流感的骨髓树突状细胞,促进了感染流感病毒的幼鼠对NP特异性CD8+ T细胞的反应,并提高了病毒清除率。最后,在多肽疫苗接种过程中,幼崽对 PA(224-233)有反应,而对 NP(366-374)没有反应。接种过 PA (224-233) 疫苗的小鼠在病毒挑战中没有保护作用。在设计靶向 T 细胞的疫苗时,如果目标患者群体包括婴儿和成人,则应考虑表位的使用。
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The Altered Neonatal CD8+ T Cell Immunodominance Hierarchy during Influenza Virus Infection Impacts Peptide Vaccination
Neonates are more susceptible to influenza virus infection than adults, resulting in increased morbidity and mortality and delayed clearance of the virus. Generating effective CD8+ T cell responses may be important for improving vaccination outcomes in vulnerable populations, but neonatal T cells frequently respond differently than adult cells. We sought to understand CD8+ T cell specificity and immunodominance during neonatal influenza infection and how any differences from the adult hierarchy might impact peptide vaccine effectiveness. Neonatal C57BL/6 mice displayed an altered CD8+ T cell immunodominance hierarchy during influenza infection, preferentially responding to an epitope in the influenza protein PA rather than the co-dominant adult response to NP and PA. Heterosubtypic infections in mice first infected as pups also displayed altered immunodominance and reduced protection compared to mice first infected as adults. Adoptive transfer of influenza-infected bone-marrow-derived dendritic cells promoted an NP-specific CD8+ T cell response in influenza-virus-infected pups and increased viral clearance. Finally, pups responded to PA (224–233), but not NP (366–374) during peptide vaccination. PA (224–233)-vaccinated mice were not protected during viral challenge. Epitope usage should be considered when designing vaccines that target T cells when the intended patient population includes infants and adults.
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