Abstract
Ageing is characterised by cellular senescence, leading to imbalanced tissue maintenance, cell death and compromised organ function. This is first observed in the thymus, the primary lymphoid organ that generates and selects T cells. However, the molecular and cellular mechanisms underpinning these ageing processes remain unclear. Here, we show that mouse ageing leads to less efficient T cell selection, decreased self-antigen representation and increased T cell receptor repertoire diversity. Using a combination of single-cell RNA-seq and lineage-tracing, we find that progenitor cells are the principal targets of ageing, whereas the function of individual mature thymic epithelial cells is compromised only modestly. Specifically, an early-life precursor cell population, retained in the mouse cortex postnatally, is virtually extinguished at puberty. Concomitantly, a medullary precursor cell quiesces, thereby impairing maintenance of the medullary epithelium. Thus, ageing disrupts thymic progenitor differentiation and impairs the core immunological functions of the thymus.
Highlights
Ageing compromises the function of vital organs via alterations of cell type composition and function (Lopez-Otın et al, 2013)
We have demonstrated how age re-models the thymic stromal scaffold and alters thymocyte composition impairing the core immunological function of the thymus
The combination of overall reduction in medullary TEC (mTEC) cellularity and the decline in promiscuous gene expression (PGE) of tissue restricted antigen-genes (TRAs) likely reduces the efficiency of antigen presentation impacting negative selection which, in turn, results in an increase in T cell receptor (TCR) repertoire diversity with age
Summary
Ageing compromises the function of vital organs via alterations of cell type composition and function (Lopez-Otın et al, 2013). The ageing process is characterised by an upregulation of immune-system-associated pathways, referred to as inflamm-ageing, which is a conserved feature across tissues and species (Benayoun et al, 2019). Ageing of the immune system first manifests as a dramatic involution of the thymus. This is the primary lymphoid organ that generates and selects a stock of immunocompetent T cells displaying an antigen receptor repertoire purged of pathogenic ‘Self’ specificities, a process known as negative selection, yet still able to react to injurious ‘Non-Self’ antigens (Palmer, 2013).
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