Transcriptomic analysis of the innate immune signatures of a SARS-CoV-2 protein subunit vaccine ZF2001 and an mRNA vaccine RRV.

IF 1.9 Q2 COMMUNICATION
Qian Wang, Ziyang Song, Jinghuan Yang, Qian He, Qunying Mao, Yu Bai, Jianyang Liu, Chaoqiang An, Xujia Yan, Bopei Cui, Lifang Song, Dong Liu, Miao Xu, Zhenglun Liang
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引用次数: 12

Abstract

Analysis of large-scale gene expression post vaccination can provide an overview of immune responses. We used transcriptional approaches to comprehensively analyze the innate immune response signatures elicited by protein subunit (PS) vaccine ZF2001 and an mRNA vaccine named RRV. A fine-grained time-dependent dissection of large-scale gene expression post immunization revealed that ZF001 induced MHC class II-related genes, including cd74 and H2-Aa, more expeditiously than the RRV. Notably, the RRV induced MHC class I-related genes such as Tap1/2, B2m, and H2-D1/K1. At day 21 post immunization, the titres of binding and neutralization antibody (NAb) induced by both vaccines were comparable, which were accordant with the expression level of genes essential to BCR/TCR signalling transduction and B/T cells activation at day 7. However, compared to ZF2001, the early responses of RRV were more robust, including the activation of pattern recognition receptors (PRRs), expression of genes involved in RNA degradation, and transcription inhibition, which are directly related to anti-viral signals. This pattern also coincided with the induction of cytokines by the RRV. Generally, the transcriptomic patterns of two very different vaccines mapped here provide a framework for establishing correlates between the induction of genes and protection, which can be tailored for evoking specific and potent immune responses against SARS-CoV-2.

对 SARS-CoV-2 蛋白亚单位疫苗 ZF2001 和 mRNA 疫苗 RRV 的先天免疫特征进行转录组学分析。
疫苗接种后的大规模基因表达分析可提供免疫反应的概况。我们利用转录方法全面分析了蛋白亚单位(PS)疫苗ZF2001和一种名为RRV的mRNA疫苗引起的先天性免疫反应特征。免疫后大规模基因表达的细粒度时间依赖性分析表明,ZF001比RRV更快诱导MHC II类相关基因,包括cd74和H2-Aa。值得注意的是,RRV诱导的是MHC I类相关基因,如Tap1/2、B2m和H2-D1/K1。免疫后第 21 天,两种疫苗诱导的结合抗体和中和抗体(NAb)滴度相当,这与第 7 天 BCR/TCR 信号转导和 B/T 细胞活化所必需的基因的表达水平相符。然而,与 ZF2001 相比,RRV 的早期反应更强,包括模式识别受体(PRR)的激活、参与 RNA 降解的基因表达和转录抑制,这些都与抗病毒信号直接相关。这种模式也与 RRV 诱导细胞因子的情况相吻合。总体而言,这里绘制的两种截然不同疫苗的转录组模式为建立基因诱导和保护之间的相关性提供了一个框架,可用于唤起针对 SARS-CoV-2 的特异性强效免疫反应。
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
CiteScore
2.60
自引率
0.00%
发文量
20
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