Acute Respiratory Illness Is Associated with Memory T Cell Differentiation and Other Immune Cell Changes in an Age-Associated Manner.

Shreya S Ugale, Tyson H Holmes, Sofia Maysel-Auslender, Scott D Boyd, Cornelia L Dekker, Mark M Davis, Holden T Maecker
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Abstract

Respiratory viruses such as influenza are encountered multiple times through infection and/or vaccination and thus have the potential to shape immune cell phenotypes over time. In particular, memory T cell compartments may be affected, as both CD4+ and CD8+ T cell responses likely contribute to viral control. In this study, we assessed immune phenotypes using cytometry by time of flight in the peripheral blood of 22 humans with acute respiratory illness and 22 age-matched noninfected controls. In younger infected individuals (1-19 y of age), we found decreased B and NK cell frequencies and a shift toward more effector-like CD4+ and CD8+ T cell phenotypes, compared with young healthy controls. Significant differences between noninfected and infected older individuals (30-74 y of age) were not seen. We also observed a decrease in naive CD4+ T cells and CD27+CD8+ T cells as well as an increase in effector memory CD8+ T cells and NKT cells in noninfected individuals with age. When cell frequencies were regressed against age for infected versus noninfected subjects, significant differences in trends with age were observed for multiple cell types. These included B cells and various subsets of CD4+ and CD8+ T cells. We conclude that acute respiratory illness drives T cell differentiation and decreases circulating B cell frequencies preferentially in young compared with older individuals.

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急性呼吸系统疾病与记忆性T细胞分化和其他免疫细胞的年龄相关变化有关。
流感等呼吸道病毒通过感染和/或疫苗接种多次遇到,因此有可能随着时间的推移形成免疫细胞表型。特别是,记忆性T细胞区室可能受到影响,因为CD4+和CD8+T细胞反应可能有助于病毒控制。在这项研究中,我们使用细胞术通过飞行时间评估了22名患有急性呼吸道疾病的人和22名年龄匹配的非感染对照的外周血中的免疫表型。在较年轻的感染者(1-19岁)中,我们发现与年轻的健康对照组相比,B细胞和NK细胞频率降低,并向更具效应子样CD4+和CD8+T细胞表型转变。未感染和感染的老年人(30-74岁)之间没有显著差异。我们还观察到,随着年龄的增长,未感染个体的初始CD4+T细胞和CD27+CD8+T细胞减少,效应记忆CD8+T细胞及NKT细胞增加。当感染和未感染受试者的细胞频率随年龄回归时,观察到多种细胞类型随年龄的趋势存在显著差异。这些细胞包括B细胞和CD4+和CD8+T细胞的各种亚群。我们得出的结论是,与老年人相比,急性呼吸系统疾病在年轻人中优先驱动T细胞分化并降低循环B细胞频率。
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