Biased Generation and In Situ Activation of Lung Tissue–Resident Memory CD4 T Cells in the Pathogenesis of Allergic Asthma

Turner, Damian; Goldklang, Monica; Cvetkovski, Filip; Paik, Daniel H; Trischler, Jordis; Barahona, Josselyn; Cao, Minwei; Dave, Ronak; Tanna, Nicole; DʼArmiento, Jeanine; Farber, Donna L.

doi:10.4049/jimmunol.1700257

Cited by 95 publications

(103 citation statements)

References 49 publications

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“…180,181 In response to prolonged allergen exposure, a similar CD69 + and Th2-biased CD4 + T RM population persists in the lung parenchyma. 182 Even in the absence of circulating T cells, these CD4 + T RM s are sufficient to mount a robust recall response. Similar autologous recall response has also been observed for helminth-induced lung CD4 + T RM s after T cell migration has been blocked.…”

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

Tissue-Specific Control of Tissue-Resident Memory T Cells

Liu

Zhang

2018

Crit Rev Immunol

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Tissue-resident memory T (TRM) cells have emerged to be a major component of T cell biology. Recent investigations have greatly advanced our understanding of TRMs. Common features have been discovered to distinguish memory T cells residing in various mucosal and non-mucosal tissues from their circulating counterparts. Given that most organs and tissues contain unique microenvironment, local signal-induced tissue-specific features are tightly associated with the differentiation, homeostasis and protective functions of TRMs. We will discuss the recent advances in TRM field with a special emphasis on the interaction between local signals and TRM cells in the context of individual tissue environment.

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Section: Cd4+ Trm Cellsmentioning

confidence: 99%

Tissue-Specific Control of Tissue-Resident Memory T Cells

Liu

Zhang

2018

Crit Rev Immunol

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“…These results suggest a possible antagonistic relationship between T RM and memory T FH cells, and highlight a role for TFs in directing the development of tissue‐resident populations. In another study using the HDM model, lung CD4 + T RM clustered around the airways at rest and rapidly reactivated upon secondary exposure within their clusters to produce IL‐4, IL‐5 and IL‐17 and recruit dendritic cells . Additional studies highlight a role for IL‐7, along with IL‐2, in the maintenance of allergen‐specific CD4 + T RM cells in the lung parenchyma and airways.…”

Section: Tissue‐resident Cd4+ Memory T‐cellsmentioning

confidence: 97%

“…In another study using the HDM model, lung CD4 + T RM clustered around the airways at rest and rapidly reactivated upon secondary exposure within their clusters to produce IL-4, IL-5 and IL-17 and recruit dendritic cells. 50 Additional studies highlight a role for IL-7, along with IL-2, in the maintenance of allergen-specific CD4 + T RM cells in the lung parenchyma and airways. However, these IL-7-dependent CD4 + T RM did not express CD69, 52 suggesting either that CD69 may not be a conclusive marker for CD4 + T RM or that CD4 + T RM are highly heterogeneous, and further studies must focus on elucidating the different subsets.…”

Section: 51mentioning

confidence: 98%

“…This may be an optimized way for helper T RM cells to perform their ‘sense‐and‐alarm’ function, initiating the innate response to recruit circulating cells and activating CD8 + T‐cells to fight off pathogen. Additionally, cytokines appear to be critical in the recruitment, formation and maintenance of CD4 + T RM in many tissues . However, which cytokines are important for which tissues remain unknown, although IL‐2 may play a key role for all T RM given its known effects in circulating memory populations .…”

Section: Tissue‐resident Cd4+ Memory T‐cellsmentioning

confidence: 99%

“…Much like circulating CD4 + memory T-cells, studies of tissue-resident lymphocytes have predominantly focused on CD8 + T RM due to the heterogeneity of CD4 + memory T-cells and the existing gaps in knowledge regarding mechanisms governing memory CD4 + T-cell formation. Nevertheless, recent studies have highlighted a prominent population of long-lived CD4 + T-cells within many nonlymphoid tissues, including the lungs, 36,[49][50][51][52][53][54][55][56][57] small intestine (SI), 12,18,[58][59][60] skin, 15,[61][62][63][64] and female reproductive tract (FRT) 18,65,66 (Fig. 2).…”

Section: Tissue-resident Cd4 + Memory T-cellsmentioning

confidence: 99%

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Origins of CD4⁺ circulating and tissue‐resident memory T‐cells

et al. 2019

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Summary In response to infection, naive CD4+ T‐cells proliferate and differentiate into several possible effector subsets, including conventional T helper effector cells (TH1, TH2, TH17), T regulatory cells (Treg) and T follicular helper cells (TFH). Once infection is cleared, a small population of long‐lived memory cells remains that mediate immune defenses against reinfection. Memory T lymphocytes have classically been categorized into central memory cell (TCM) and effector memory cell (TEM) subsets, both of which circulate between blood, secondary lymphoid organs and in some cases non‐lymphoid tissues. A third subset of memory cells, referred to as tissue‐resident memory cells (TRM), resides in tissues without recirculation, serving as ‘first line’ of defense at barrier sites, such as skin, lung and intestinal mucosa, and augmenting innate immunity in the earliest phases of reinfection and recruiting circulating CD4+ and CD8+ T‐cells. The presence of multiple CD4+ T helper subsets has complicated studies of CD4+ memory T‐cell differentiation, and the mediators required to support their function. In this review, we summarize recent investigations into the origins of CD4+ memory T‐cell populations and discuss studies addressing CD4+ TRM differentiation in barrier tissues.

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Tissue resident T cell memory or how the magnificent seven are chilling in the bone

Zens

Münz

2019

Eur J Immunol

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Following infection, tissue-resident memory T cells (Trm) are thought to be left behind atsites of antigen encounter to protect affected tissues against subsequent reinfection. In this issue of the European Journal of Immunology, however, Pascutti et al. demonstrate that both murine and human CD8 + Trm specific to seven different pathogens, including systemic, skin, and lung tissue-localized pathogens, accumulate in the bone marrow (BM). These cells have a CD69 + phenotype, develop independently of local antigen, and require IL-15, Blimp-1, and Hobit for their differentiation and maintenance. Following restimulation, these cells expand and rapidly produce cytokines. While some of these responses may protect the BM from infection, the consideration that some of these pathogens or their antigens might never reach the BM suggests additional functional roles of BM Trm, possibly in supporting hematopoietic functions via cytokine production following infection. It will be further interesting to determine whether BM Trm contribute to the circulating effector pool following reinfection with tissue-localized or systemic pathogens and whether these cells can be elicited by vaccination. Keywords: Blimp-1 r bone marrow r Hobit r IL-15 r tissue resident memory T cells See accompanying article by Pascutti et al. References 1 Sallusto, F., Lenig, D., Forster, R., Lipp, M. and Lanzavecchia, A., Two subsets of memory T lymphocytes with distinct homing potentials and effector functions.

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Biased Generation and In Situ Activation of Lung Tissue–Resident Memory CD4 T Cells in the Pathogenesis of Allergic Asthma

Cited by 95 publications

References 49 publications

Tissue-Specific Control of Tissue-Resident Memory T Cells

Tissue-Specific Control of Tissue-Resident Memory T Cells

Origins of CD4⁺ circulating and tissue‐resident memory T‐cells

Tissue resident T cell memory or how the magnificent seven are chilling in the bone

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Biased Generation and In Situ Activation of Lung Tissue–Resident Memory CD4 T Cells in the Pathogenesis of Allergic Asthma

Cited by 95 publications

References 49 publications

Tissue-Specific Control of Tissue-Resident Memory T Cells

Tissue-Specific Control of Tissue-Resident Memory T Cells

Origins of CD4+ circulating and tissue‐resident memory T‐cells

Tissue resident T cell memory or how the magnificent seven are chilling in the bone

Contact Info

Product

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Origins of CD4⁺ circulating and tissue‐resident memory T‐cells