Metabolic characteristics of CD8+ T cell subsets in young and aged individuals are not predictive of functionality

Author:

Quinn Kylie M.ORCID,Hussain TabindaORCID,Kraus Felix,Formosa Luke E.ORCID,Lam Wai K.ORCID,Dagley Michael J.ORCID,Saunders Eleanor C.,Assmus Lisa M.ORCID,Wynne-Jones Erica,Loh LiyenORCID,van de Sandt Carolien E.ORCID,Cooper LucyORCID,Good-Jacobson Kim L.ORCID,Kedzierska KatherineORCID,Mackay Laura K.ORCID,McConville Malcolm J.ORCID,Ramm GeorgORCID,Ryan Michael T.ORCID,La Gruta Nicole L.ORCID

Abstract

AbstractVirtual memory T (TVM) cells are antigen-naïve CD8+ T cells that exist in a semi-differentiated state and exhibit marked proliferative dysfunction in advanced age. High spare respiratory capacity (SRC) has been proposed as a defining metabolic characteristic of antigen-experienced memory T (TMEM) cells, facilitating rapid functionality and survival. Given the semi-differentiated state of TVM cells and their altered functionality with age, here we investigate TVM cell metabolism and its association with longevity and functionality. Elevated SRC is a feature of TVM, but not TMEM, cells and it increases with age in both subsets. The elevated SRC observed in aged mouse TVM cells and human CD8+ T cells from older individuals is associated with a heightened sensitivity to IL-15. We conclude that elevated SRC is a feature of TVM, but not TMEM, cells, is driven by physiological levels of IL-15, and is not indicative of enhanced functionality in CD8+ T cells.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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