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Publication : Comparative analysis reveals a role for TGF-β in shaping the residency-related transcriptional signature in tissue-resident memory CD8+ T cells.

First Author  Nath AP Year  2019
Journal  PLoS One Volume  14
Issue  2 Pages  e0210495
PubMed ID  30742629 Mgi Jnum  J:272272
Mgi Id  MGI:6280252 Doi  10.1371/journal.pone.0210495
Citation  Nath AP, et al. (2019) Comparative analysis reveals a role for TGF-beta in shaping the residency-related transcriptional signature in tissue-resident memory CD8+ T cells. PLoS One 14(2):e0210495
abstractText  Tissue-resident CD8+ memory T (TRM) cells are immune cells that permanently reside at tissue sites where they play an important role in providing rapid protection against reinfection. They are not only phenotypically and functionally distinct from their circulating memory counterparts, but also exhibit a unique transcriptional profile. To date, the local tissue signals required for their development and long-term residency are not well understood. So far, the best-characterised tissue-derived signal is transforming growth factor-beta (TGF-beta), which has been shown to promote the development of these cells within tissues. In this study, we aimed to determine to what extent the transcriptional signatures of TRM cells from multiple tissues reflects TGF-beta imprinting. We activated murine CD8+ T cells, stimulated them in vitro by TGF-beta, and profiled their transcriptomes using RNA-seq. Upon comparison, we identified a TGF-beta-induced signature of differentially expressed genes between TGF-beta-stimulated and -unstimulated cells. Next, we linked this in vitro TGF-beta-induced signature to a previously identified in vivo TRM-specific gene set and found considerable (>50%) overlap between the two gene sets, thus showing that a substantial part of the TRM signature can be attributed to TGF-beta signalling. Finally, gene set enrichment analysis further revealed that the altered gene signature following TGF-beta exposure reflected transcriptional signatures found in TRM cells from both epithelial and non-epithelial tissues. In summary, these findings show that TGF-beta has a broad footprint in establishing the residency-specific transcriptional profile of TRM cells, which is detectable in TRM cells from diverse tissues. They further suggest that constitutive TGF-beta signaling might be involved for their long-term persistence at tissue sites.
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