| Literature DB >> 26682984 |
Laura K Mackay1, Erica Wynne-Jones2, David Freestone2, Daniel G Pellicci3, Lisa A Mielke4, Dane M Newman2, Asolina Braun2, Frederick Masson5, Axel Kallies4, Gabrielle T Belz4, Francis R Carbone2.
Abstract
Tissue-resident memory T (Trm) cells contribute to local immune protection in non-lymphoid tissues such as skin and mucosa, but little is known about their transcriptional regulation. Here we showed that CD8(+)CD103(+) Trm cells, independent of circulating memory T cells, were sufficient for protection against infection and described molecular elements that were crucial for their development in skin and lung. We demonstrated that the T-box transcription factors (TFs) Eomes and T-bet combined to control CD8(+)CD103(+) Trm cell formation, such that their coordinate downregulation was crucial for TGF-β cytokine signaling. TGF-β signaling, in turn, resulted in reciprocal T-box TF downregulation. However, whereas extinguishment of Eomes was necessary for CD8(+)CD103(+) Trm cell development, residual T-bet expression maintained cell surface interleukin-15 (IL-15) receptor β-chain (CD122) expression and thus IL-15 responsiveness. These findings indicate that the T-box TFs control the two cytokines, TGF-β and IL-15, which are pivotal for CD8(+)CD103(+) Trm cell development and survival.Entities:
Keywords: T-box transcription factors; TGF-β; Tissue-resident memory T cells; peripheral immunity
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Year: 2015 PMID: 26682984 DOI: 10.1016/j.immuni.2015.11.008
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745