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Publication : Cognate antigen engagement on parenchymal cells stimulates CD8<sup>+</sup> T cell proliferation in situ.

First Author  Sutherland RM Year  2017
Journal  Nat Commun Volume  8
Pages  14809 PubMed ID  28401883
Mgi Jnum  J:273655 Mgi Id  MGI:5921550
Doi  10.1038/ncomms14809 Citation  Sutherland RM, et al. (2017) Cognate antigen engagement on parenchymal cells stimulates CD8+ T cell proliferation in situ. Nat Commun 8:14809
abstractText  T-cell responses are initiated upon cognate presentation by professional antigen presenting cells in lymphoid tissue. T cells then migrate to inflamed tissues, but further T-cell stimulation in these parenchymal target sites is not well understood. Here we show that T-cell expansion within inflamed tissues is a distinct phase that is neither a classical primary nor classical secondary response. This response, which we term 'the mezzanine response', commences within days after initial antigen encounter, unlike the secondary response that usually occurs weeks after priming. A further distinction of this response is that T-cell proliferation is driven by parenchymal cell antigen presentation, without requiring professional antigen presenting cells, but with increased dependence on IL-2. The mezzanine response might, therefore, be a new target for inhibiting T-cell responses in allograft rejection and autoimmunity or for enhancing T-cell responses in the context of microbial or tumour immunity.
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