Local and systemic responses to SARS-CoV-2 infection in children and adults

干扰素 免疫学 免疫系统 先天免疫系统 医学 细胞毒性T细胞 病毒复制 病毒 生物 病毒学 遗传学 体外
作者
Masahiro Yoshida,Kaylee B. Worlock,Ni Huang,Rik G.H. Lindeboom,Colin R. Butler,Natsuhiko Kumasaka,Cecilia Domínguez Conde,Lira Mamanova,Liam Bolt,Laura Richardson,Krzysztof Polański,Elo Madissoon,Josephine L. Barnes,Jessica Allen-Hyttinen,Eliz Kilich,Brendan C. Jones,Angus de Wilton,Anna Wilbrey-Clark,Waradon Sungnak,J. Patrick Pett,Juliane Weller,Elena Prigmore,Henry Yung,Puja Mehta,Aarash Saleh,Anita Saigal,Vivian Chu,Jonathan Cohen,Clare Cane,Aikaterini Iordanidou,Soichi Shibuya,Ann‐Kathrin Reuschl,Iván T. Herczeg,A. Christine Argento,Richard G. Wunderink,Sean B. Smith,Taylor A. Poor,Catherine A. Gao,Jane E. Dematte,G. R. Scott Budinger,Helen K. Donnelly,Nikolay S. Markov,Ziyan Lu,Gary Reynolds,Muzlifah Haniffa,Georgina Bowyer,Matthew Coates,Menna R. Clatworthy,Fernando J. Calero‐Nieto,Berthold Göttgens,Christopher O’Callaghan,Neil J. Sebire,Clare Jolly,Paolo De Coppi,Claire M. Smith,Alexander V. Misharin,Sam M. Janes,Sarah A. Teichmann,Marko Nikolić,Kerstin B. Meyer
出处
期刊:Nature [Nature Portfolio]
卷期号:602 (7896): 321-327 被引量:222
标识
DOI:10.1038/s41586-021-04345-x
摘要

Abstract It is not fully understood why COVID-19 is typically milder in children 1–3 . Here, to examine the differences between children and adults in their response to SARS-CoV-2 infection, we analysed paediatric and adult patients with COVID-19 as well as healthy control individuals (total n = 93) using single-cell multi-omic profiling of matched nasal, tracheal, bronchial and blood samples. In the airways of healthy paediatric individuals, we observed cells that were already in an interferon-activated state, which after SARS-CoV-2 infection was further induced especially in airway immune cells. We postulate that higher paediatric innate interferon responses restrict viral replication and disease progression. The systemic response in children was characterized by increases in naive lymphocytes and a depletion of natural killer cells, whereas, in adults, cytotoxic T cells and interferon-stimulated subpopulations were significantly increased. We provide evidence that dendritic cells initiate interferon signalling in early infection, and identify epithelial cell states associated with COVID-19 and age. Our matching nasal and blood data show a strong interferon response in the airways with the induction of systemic interferon-stimulated populations, which were substantially reduced in paediatric patients. Together, we provide several mechanisms that explain the milder clinical syndrome observed in children.

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