CD4+ T cells persist for years in the human small intestine and mediate robust TH1 immunity

Author:

Casado Raquel BartoloméORCID,Landsverk Ole J.B.ORCID,Chauhan Sudhir KumarORCID,Sætre FrankORCID,Hagen Kjersti ThorvaldsenORCID,Yaqub SherazORCID,Øyen OleORCID,Horneland RuneORCID,Aandahl Einar MartinORCID,Aabakken LarsORCID,Bækkevold Espen S.ORCID,Jahnsen Frode L.ORCID

Abstract

AbstractStudies in mice and humans have shown that CD8+ T cell immunosurveillance in non-lymphoid tissues is dominated by resident populations. Whether CD4+ T cells use the same strategies to survey peripheral tissues is less clear. Here, examining the turnover of CD4+ T cells in transplanted duodenum in humans, we demonstrate that the majority of CD4+ T cells were still donor-derived one year after transplantation. In contrast to memory CD4+ T cells in peripheral blood, intestinal CD4+ TRM cells expressed CD69 and CD161, but only a minor fraction expressed CD103. Functionally, intestinal CD4+ TRM cells were very potent cytokine producers; the vast majority being polyfunctional TH1 cells, whereas a minor fraction produced IL-17. Interestingly, a fraction of intestinal CD4+ T cells produced granzyme-B and perforin after activation. Together, we show that the intestinal CD4+ T-cell compartment is dominated by resident populations that survive for more than 1 year. This finding is of high relevance for the development of oral vaccines and therapies for diseases in the gut.

Publisher

Cold Spring Harbor Laboratory

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