Longitudinal single-cell immune profiling revealed distinct innate immune response in asymptomatic COVID-19 patients

Author:

Zhao Xiang-Na,You YueORCID,Wang Guo-Lin,Gao Hui-Xia,Cui Xiao-Ming,Duan Li-Jun,Zhang Sheng-Bo,Wang Yu-Ling,Lin-Yao ,Li Li,Lu Jian-Hua,Wang Hai-Bin,Fan Jing-Fang,Zheng Huan-Wei,Dai Er-Hei,Tian Lu-Yi,Ma Mai-Juan

Abstract

SUMMARYRecent studies have characterized the single-cell immune landscape of host immune response of coronavirus disease 2019 (COVID-19), specifically focus on the severe condition. However, the immune response in mild or even asymptomatic patients remains unclear. Here, we performed longitudinal single-cell transcriptome sequencing and T cell/B cell receptor sequencing on 3 healthy donors and 10 COVID-19 patients with asymptomatic, moderate, and severe conditions. We found asymptomatic patients displayed distinct innate immune responses, including increased CD56briCD16NK subset, which was nearly missing in severe condition and enrichment of a new Th2-like cell type/state expressing a ciliated cell marker. Unlike that in moderate condition, asymptomatic patients lacked clonal expansion of effector CD8+T cells but had a robust effector CD4+T cell clonal expansion, coincide with previously detected SARS-CoV-2-reactive CD4+T cells in unexposed individuals. Moreover, NK and effector T cells in asymptomatic patients have upregulated cytokine related genes, such asIFNGandXCL2. Our data suggest early innate immune response and type I immunity may contribute to the asymptomatic phenotype in COVID-19 disease, which could in turn deepen our understanding of severe COVID-19 and guide early prediction and therapeutics.

Publisher

Cold Spring Harbor Laboratory

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