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Systems biology of immunity to MF59-adjuvanted versus nonadjuvanted trivalent seasonal influenza vaccines in early childhood.

机译:儿童早期对MF59佐剂与非佐剂三价季节性流感疫苗免疫的系统生物学。

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摘要

The dynamics and molecular mechanisms underlying vaccine immunity in early childhood remain poorly understood. Here we applied systems approaches to investigate the innate and adaptive responses to trivalent inactivated influenza vaccine (TIV) and MF59-adjuvanted TIV (ATIV) in 90 14- to 24-mo-old healthy children. MF59 enhanced the magnitude and kinetics of serum antibody titers following vaccination, and induced a greater frequency of vaccine specific, multicytokine-producing CD4(+) T cells. Compared with transcriptional responses to TIV vaccination previously reported in adults, responses to TIV in infants were markedly attenuated, limited to genes regulating antiviral and antigen presentation pathways, and observed only in a subset of vaccinees. In contrast, transcriptional responses to ATIV boost were more homogenous and robust. Interestingly, a day 1 gene signature characteristic of the innate response (antiviral IFN genes, dendritic cell, and monocyte responses) correlated with hemagglutination at day 28. These findings demonstrate that MF59 enhances the magnitude, kinetics, and consistency of the innate and adaptive response to vaccination with the seasonal influenza vaccine during early childhood, and identify potential molecular correlates of antibody responses.
机译:对儿童早期疫苗免疫的动力学和分子机制仍然知之甚少。在这里,我们应用系统方法研究了90名14至24岁健康儿童对三价灭活流感疫苗(TIV)和MF59辅助TIV(ATIV)的先天性和适应性反应。 MF59增强了接种疫苗后血清抗体滴度的大小和动力学,并诱导了更高的疫苗特异性多细胞因子产生CD4(+)T细胞频率。与先前报道的成人对TIV疫苗的转录反应相比,婴儿对TIV的反应明显减弱,仅限于调节抗病毒和抗原呈递途径的基因,并且仅在一部分疫苗中观察到。相反,对ATIV增强的转录反应更为同质和稳健。有趣的是,先天应答(抗病毒IFN基因,树突状细胞和单核细胞应答)的第1天基因特征与第28天的血凝相关。这些发现表明MF59增强了先天应答和适应性应答的强度,动力学和一致性。在儿童早期接种季节性流感疫苗,并确定抗体反应的潜在分子相关性。

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