2014
DOI: 10.1371/journal.ppat.1004210
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Toll-Like Receptor 8 Agonist and Bacteria Trigger Potent Activation of Innate Immune Cells in Human Liver

Abstract: The ability of innate immune cells to sense and respond to impending danger varies by anatomical location. The liver is considered tolerogenic but is still capable of mounting a successful immune response to clear various infections. To understand whether hepatic immune cells tune their response to different infectious challenges, we probed mononuclear cells purified from human healthy and diseased livers with distinct pathogen-associated molecules. We discovered that only the TLR8 agonist ssRNA40 selectively … Show more

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Cited by 207 publications
(228 citation statements)
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“…MAIT cells are only a small fraction of the CD161++ CD8+ T‐cell population in cord blood,83 but slowly expand with age, making up more than 90% of the CD161++ CD8+ T‐cell population in adults 11, 14. Both MAIT and non‐MAIT CD161++ CD8+ T‐cells share functional features, most notably the ability to respond to innate cytokines in the absence of TCR stimulation, due to their high expression of cytokine receptors such as IL‐18R and IL‐12R 9, 84. This function is likely driven by the shared expression by MAIT and non‐MAIT CD161++ CD8+ T‐cells of the master transcription factor promyelocytic leukaemia zinc finger protein (PLZF) 14, 85…”
Section: Subsets Of Cd8+ T‐cellsmentioning
confidence: 99%
“…MAIT cells are only a small fraction of the CD161++ CD8+ T‐cell population in cord blood,83 but slowly expand with age, making up more than 90% of the CD161++ CD8+ T‐cell population in adults 11, 14. Both MAIT and non‐MAIT CD161++ CD8+ T‐cells share functional features, most notably the ability to respond to innate cytokines in the absence of TCR stimulation, due to their high expression of cytokine receptors such as IL‐18R and IL‐12R 9, 84. This function is likely driven by the shared expression by MAIT and non‐MAIT CD161++ CD8+ T‐cells of the master transcription factor promyelocytic leukaemia zinc finger protein (PLZF) 14, 85…”
Section: Subsets Of Cd8+ T‐cellsmentioning
confidence: 99%
“…These results demonstrated the therapeutic implications of TLR8 agonists for the treatment of chronic liver infections. 80 Therefore, TLR3, 7 and 8 agonists are promising drug candidates for the treatment of chronic HBV infection if their toxicity can be reduced to a tolerated range.…”
Section: Using Tlr Agonists For Immunotherapy In Chronic Hbv Infectionmentioning
confidence: 99%
“…We and others have characterized the cell populations flushed from the sinusoids of the healthy liver and showed significant variation in cellular content and cytokine profiles compared with PBMCs. [50][51][52] However, almost no information is available to compare the differences in these populations between HBV patients and healthy donors. Analyses of HBV-infected livers are often restricted to biopsy-sized samples or are explants due to advanced disease; as such, the processes required to extract cells are quite harsh, possibly interfering with or inhibiting downstream analysis.…”
Section: Areas Of Further Investigationmentioning
confidence: 99%