Marked T cell activation, senescence, exhaustion and skewing towards TH17 in patients with COVID-19 pneumonia.

Sara De BiasiMarianna MeschiariLara GibelliniCaterina BellinazziRebecca BorellaLucia FidanzaLicia GozziAnna IannoneDomenico Lo Tartaro Marco MattioliAnnamaria PaoliniMarianna MenozziJovana MilićGiacomo FranceschiRiccardo FantiniRoberto TonelliMarco SitaMario SartiTommaso TrentiLucio BrugioniLuca CicchettiFabio Facchinetti Antonello Pietrangelo Enrico Maria CliniMassimo GirardisGiovanni GuaraldiCristina MussiniAndrea Cossarizza

Published in: Nature communications (2020)

The immune system of patients infected by SARS-CoV-2 is severely impaired. Detailed investigation of T cells and cytokine production in patients affected by COVID-19 pneumonia are urgently required. Here we show that, compared with healthy controls, COVID-19 patients' T cell compartment displays several alterations involving naïve, central memory, effector memory and terminally differentiated cells, as well as regulatory T cells and PD1+CD57+ exhausted T cells. Significant alterations exist also in several lineage-specifying transcription factors and chemokine receptors. Terminally differentiated T cells from patients proliferate less than those from healthy controls, whereas their mitochondria functionality is similar in CD4+ T cells from both groups. Patients display significant increases of proinflammatory or anti-inflammatory cytokines, including T helper type-1 and type-2 cytokines, chemokines and galectins; their lymphocytes produce more tumor necrosis factor (TNF), interferon-γ, interleukin (IL)-2 and IL-17, with the last observation implying that blocking IL-17 could provide a novel therapeutic strategy for COVID-19.

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