Regulatory KIR+ RA+ T cells accumulate with age and are highly activated during viral respiratory disease.
Daan K J PierenNoortje A M SmitsJeroen HoeboerVinitha KandiahRimke J PostelRob MarimanJosine van BeekDebbie van BaarleJelle de WitTeun GuichelaarPublished in: Aging cell (2021)
Severe respiratory viral infectious diseases such as influenza and COVID-19 especially affect the older population. This is partly ascribed to diminished CD8+ T-cell responses a result of aging. The phenotypical diversity of the CD8+ T-cell population has made it difficult to identify the impact of aging on CD8+ T-cell subsets associated with diminished CD8+ T-cell responses. Here we identify a novel human CD8+ T-cell subset characterized by expression of Killer-cell Immunoglobulin-like Receptors (KIR+ ) and CD45RA (RA+ ). These KIR+ RA+ T cells accumulated with age in the blood of healthy individuals (20-82 years of age, n = 50), expressed high levels of aging-related markers of T-cell regulation, and were functionally capable of suppressing proliferation of other CD8+ T cells. Moreover, KIR+ RA+ T cells were a major T-cell subset becoming activated in older adults suffering from an acute respiratory viral infection (n = 36), including coronavirus and influenza virus infection. In addition, older adults with influenza A infection showed that higher activation status of their KIR+ RA+ T cells associated with longer duration of respiratory symptoms. Together, our data indicate that KIR+ RA+ T cells are a unique human T-cell subset with regulatory properties that may explain susceptibility to viral respiratory disease at old age.
Keyphrases
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- endothelial cells
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- infectious diseases
- interstitial lung disease
- transcription factor
- coronavirus disease
- systemic lupus erythematosus
- liver failure
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- induced pluripotent stem cells
- systemic sclerosis
- stem cells
- respiratory tract
- peripheral blood
- deep learning
- early onset
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