Author: Xie, Min; Yunis, Joseph; Yao, Yin; Shi, Jing; Yang, Yang; Zhou, Pengcheng; Liang, Kaili; Wan, Yanmin; Mehdi, Ahmed; Chen, Zhian; Wang, Naiqi; Xu, Shuyun; Zhou, Min; Yu, Muqing; Wang, Ke; Tao, Yu; Zhou, Ying; Li, Xiaochen; Liu, Xiansheng; Yu, Xiao; Wei, Yunbo; Liu, Zheng; Sprent, Jonathan; Yu, Di
Title: High levels of soluble CD25 in COVIDâ€19 severity suggest a divergence between antiâ€viral and proâ€inflammatory Tâ€cell responses Cord-id: o5ly74nq Document date: 2021_2_15
ID: o5ly74nq
Snippet: OBJECTIVES: We aimed to gain an understanding of the paradox of the immunity in COVIDâ€19 patients with T cells showing both functional defects and hyperactivation and enhanced proliferation. METHODS: A total of 280 hospitalised patients with COVIDâ€19 were evaluated for cytokine profiles and clinical features including viral shedding. A mouse model of acute infection by lymphocytic choriomeningitis virus (LCMV) was applied to dissect the relationship between immunological, virological and pat
Document: OBJECTIVES: We aimed to gain an understanding of the paradox of the immunity in COVIDâ€19 patients with T cells showing both functional defects and hyperactivation and enhanced proliferation. METHODS: A total of 280 hospitalised patients with COVIDâ€19 were evaluated for cytokine profiles and clinical features including viral shedding. A mouse model of acute infection by lymphocytic choriomeningitis virus (LCMV) was applied to dissect the relationship between immunological, virological and pathological features. The results from the mouse model were validated by published data set of singleâ€cell RNA sequencing (scRNAâ€seq) of immune cells in bronchoalveolar lavage fluid (BALF) of COVIDâ€19 patients. RESULTS: The levels of soluble CD25 (sCD25), ILâ€6, ILâ€8, ILâ€10 and TNFâ€Î± were higher in severe COVIDâ€19 patients than nonâ€severe cases, but only sCD25 was identified as an independent risk factor for disease severity by multivariable binary logistic regression analysis and showed a positive association with the duration of viral shedding. In agreement with the clinical observation, LCMVâ€infected mice with high levels of sCD25 demonstrated insufficient antiâ€viral response and delayed viral clearance. The elevation of sCD25 in mice was mainly contributed by the expansion of CD25(+)CD8(+) T cells that also expressed the highest level of PDâ€1 with proâ€inflammatory potential. The counterpart human CD25(+)PDâ€1(+) T cells were expanded in BALF of COVIDâ€19 patients with severe disease compared to those with modest disease. CONCLUSION: These results suggest that high levels of sCD25 in COVIDâ€19 patients probably result from insufficient antiâ€viral immunity and indicate an expansion of proâ€inflammatory T cells that contribute to disease severity.
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