ADAMTS5: A critical enzyme for the maintenance of influenza-specific CD8+ T cell memory

Abstract

Abstract Extracellular matrix (ECM) enzymes, such as the ADAMTS (A disintegrin-like and metalloproteinase with thrombospondin-1 motifs) family, play a significant role in ECM remodelling. ECM remodelling facilitates immune cell migration and adhesion. ADAMTS5, a member of the ADAMTS family, cleaves ECM proteoglycans, such as aggrecan and versican, and has a well-characterised role in osteoarthritis and embryogenesis. However, ADAMTS5 has an un-identified role throughout the immune response. Our previous studies indicated that ADAMTS5 expression is required to mediate T cell migration during acute influenza virus infection. In this current study, we analysed secondary acute responses (day 7) and primary memory (day 30) following influenza infection of Adamts5−/− mice. Here, we primed Adamts5−/− mice with PR8 influenza virus (1.5×107 pfu/mouse) and challenged 8 weeks later with X31 influenza virus (104 pfu/mouse). Following secondary infection, Adamts5−/− mice displayed greater weight loss and expressed fewer IFNγ+NP366-372+CD8+T cells. Critically, we observed a reduced number of influenza-specific CD8+ memory cells (CD62LhiCD44lo) in Adamts5−/− mice after primary infection, which may result in the lower number of IFNγ+NP366-372+CD8+T cells observed in secondary acute infection. We therefore hypothesize that the ADAMTS5 enzyme, through its ECM remodelling capabilities, is essential for the maintenance of memory and recall of functional immunity following secondary infection.