4.4 Article

T cell trafficking and metabolism: novel mechanisms and targets for immunomodulation

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CURRENT OPINION IN PHARMACOLOGY
卷 12, 期 4, 页码 452-457

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ELSEVIER SCI LTD
DOI: 10.1016/j.coph.2012.02.018

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  1. British Heart Foundation
  2. Medical Research Council of the UK
  3. Gates Foundation
  4. British Heart Foundation [RG/09/002/26425, FS/12/38/29640] Funding Source: researchfish

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Coordinated migratory events by naive and memory T cells are key to effective immunity. Naive T cells predominantly recirculate through secondary lymphoid tissue until antigen encounter, while primed T cells efficiently localize to antigen-rich lymphoid and non-lymphoid tissue. Tissue-selective targeting by primed T cells is achieved by a combination of inflammatory signals and tissue-selective homing receptors acquired by T cells during activation and differentiation. A large number of molecular mediators and interactions promoting memory T cell migration to non-lymphoid sites of inflammation have been identified. Recently, additional antigen-driven mechanisms have been proposed, which orchestrate the targeted delivery of memory T cells to antigen-rich tissue. Importantly, recent studies have revealed that the T cell metabolic status influences their differentiation and homing patterns. We here summarize these key observations and discuss their relevance for the manipulation of immune anatomy in therapeutic settings.

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