T cell receptor is required for differentiation but not maintenance of intestinal intraepithelial lymphocytes

Bilate, Angelina M.; London, Mariya; Castro, Tiago B. R.; Mesin, Luka; Kongthong, Suppawat; Harnagel, Audrey; Victora, Gabriel D.; Mucida, Daniel

doi:10.1101/2020.06.04.134510

Cited by 2 publications

(2 citation statements)

References 61 publications

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“…Because Cryptosporidium is restricted to IECs and does not infect professional APCs, there are basic questions about how parasite-derived antigens gain access to the mLN and whether APCs at the site of infection can acquire parasite antigens and support local CD4 + T cell function (54). Interestingly, IECs can express MHCII, and differentiation of CD4 + T cells into CD4 + CD8αα IELs within the gut requires MHCII expression on IECs (72). During Cryptosporidium infection, IFN-γ signaling on IECs leads to higher MHCII and CIITA expression (32,73 Preprint), which may facilitate the ability of IECs to engage effector CD4 + T cells within the IEL.…”

Section: Discussionmentioning

confidence: 99%

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium

Cohn,

Wallbank,

Haskins

et al. 2023

Preprint

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Cryptosporidiumis an enteric pathogen that is a prominent cause of diarrheal disease. Control of this infection requires CD4+T cells, though the processes that lead to T cell-mediated resistance have been difficult to assess. Here,Cryptosporidiumparasites that express MHCII-restricted model antigens were generated to dissect the early events that influence CD4+T cell priming and effector function. These studies highlight that parasite-specific CD4+T cells are primed in the draining mesenteric lymph node (mesLN) and differentiate into Th1 cells in the gut, where they mediate IFN-γ-dependent control of the infection. Although type 1 conventional dendritic cells (cDC1s) were not required for initial priming of CD4+T cells, cDC1s were required for CD4+T cell expansion and gut homing. cDC1s were also a major source of IL-12 that was not required for priming but promoted full differentiation of CD4+T cells and local production of IFN-γ. Together, these studies reveal distinct roles for cDC1s in shaping CD4+T cell responses to enteric infection: first to drive early expansion in the mesLN and second to drive effector responses in the gut.SummaryCryptosporidiumparasites that express model antigens were generated to dissect how parasite-specific CD4+T cells are primed and mediate effector functions required to control this enteric pathogen. cDC1s produced IL-12p40 and were required for early expansion and gut homing of CD4+T cells. However, IL-12p40 was only required for the development of Th1 CD4+T cell effector function in the gut.

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Section: Discussionmentioning

confidence: 99%

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium

Cohn,

Wallbank,

Haskins

et al. 2023

Preprint

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“…The development of CD4 + CD8αα + IELs is also affected by microbiota members, such as Lactobacillus reuteri [180]. The microbiota-driven expression of MHC-II and programmed deathligand 1 (PD-L1) by IECs is required for the differentiation of CD4 T cells to become CD4 + CD8αα + IELs [181,182].…”

Section: T Cellsmentioning

confidence: 99%

Non‐zero‐sum microbiome immune system interactions

Tuganbaev

Honda

2021

Eur J Immunol

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Fundamental asymmetries between the host and its microbiome in enzymatic activities and nutrient storage capabilities have promoted mutualistic adaptations on both sides. As a result, the enteric immune system has evolved so as not to cause a zero-sum sterilization of non-self, but rather achieve a non-zero-sum self-reinforcing cooperation with its evolutionary partner the microbiome. In this review, we attempt to integrate the accumulated knowledge of immune-microbiome interactions into an evolutionary framework and trace the pattern of positive immune-microbiome feedback loops across epithelial, enteric nervous system, innate, and adaptive immune circuits. Indeed, the immune system requires commensal signals for its development and function, and reciprocally protects the microbiome from nutrient shortage and pathogen outgrowth. In turn, a healthy microbiome is the result of immune system curatorship as well as microbial ecology. The paradigms of host-microbiome asymmetry and the cooperative nature of their interactions identified in the gut are applicable across all tissues influenced by microbial activities. Incorporation of immune system influences into models of microbiome ecology will be a step forward toward defining what constitutes a healthy human microbiome and guide discoveries of novel host-microbiome mutualistic adaptations that may be harnessed for the promotion of human health.

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T cell receptor is required for differentiation but not maintenance of intestinal intraepithelial lymphocytes

Cited by 2 publications

References 61 publications

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium

Non‐zero‐sum microbiome immune system interactions

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T cell receptor is required for differentiation but not maintenance of intestinal intraepithelial lymphocytes

Cited by 2 publications

References 61 publications

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4+T cell-mediated resistance toCryptosporidium

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4+T cell-mediated resistance toCryptosporidium

Non‐zero‐sum microbiome immune system interactions

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Product

Resources

About

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4⁺T cell-mediated resistance toCryptosporidium