| Literature DB >> 30282039 |
Lauren E Holz1, Julia E Prier2, David Freestone2, Thiago M Steiner2, Kieran English3, Darryl N Johnson4, Vanessa Mollard5, Anton Cozijnsen5, Gayle M Davey2, Dale I Godfrey4, Katsuyuki Yui6, Laura K Mackay4, Mireille H Lahoud7, Irina Caminschi7, Geoffrey I McFadden5, Patrick Bertolino3, Daniel Fernandez-Ruiz8, William R Heath9.
Abstract
Liver tissue-resident memory T (Trm) cells migrate throughout the sinusoids and are capable of protecting against malaria sporozoite challenge. To gain an understanding of liver Trm cell development, we examined various conditions for their formation. Although liver Trm cells were found in naive mice, their presence was dictated by antigen specificity and required IL-15. Liver Trm cells also formed after adoptive transfer of in vitro-activated but not naive CD8+ T cells, indicating that activation was essential but that antigen presentation within the liver was not obligatory. These Trm cells patrolled the liver sinusoids with a half-life of 36 days and occupied a large niche that could be added to sequentially without effect on subsequent Trm cell cohorts. Together, our findings indicate that liver Trm cells form as a normal consequence of CD8+ T cell activation during essentially any infection but that inflammatory and antigenic signals preferentially tailor their development.Entities:
Keywords: T cell memory; liver; liver immunology; malaria; niche; tissue-resident memory
Year: 2018 PMID: 30282039 DOI: 10.1016/j.celrep.2018.08.094
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423