IL-15 supports the generation of protective lung-resident memory CD4 T cells

Strutt, Tara M.; Dhume, Kunal; Finn, Caroline; Hwang, Ji Hae; Castonguay, Catherine; Swain, Susan L.; McKinstry, K. Kai

doi:10.1038/mi.2017.101

Cited by 77 publications

(96 citation statements)

References 53 publications

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“…27,28,67,152,177,178 Comparing with CD8 + lung T RM , CD4 + T RM cells usually carry less CD103 or express CD11a instead of CD103. 170,178,179 Genome wide transcriptional analysis reveals that CD4 + lung T RM cells resemble CD8 + lung T RM cells. 151,152,179 Similar transcription programs including the down-regulation of T-bet and Eomes, and the up-regulation of Blimp-1 and Notch signaling, direct the local differentiation of lung CD4 + T RM cells.…”

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

“…170,178,179 Genome wide transcriptional analysis reveals that CD4 + lung T RM cells resemble CD8 + lung T RM cells. 151,152,179 Similar transcription programs including the down-regulation of T-bet and Eomes, and the up-regulation of Blimp-1 and Notch signaling, direct the local differentiation of lung CD4 + T RM cells. 152 Interestingly, human and mouse infant T cells (including both CD4 + and CD8 + T cells) express enhanced levels of T-bet and exhibit defective lung T RM cell formation, further suggesting that down-regulation of T-bet is a conserved common mechanism underlying both CD4 + and CD8 + T RM differentiation.…”

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

“…Distinct from CD103 + CD8 + T RM , IL-15 is required during the early differentiation, but not the long-term maintenance of CD4 + lung T RM cells in mouse. 179 Following both acute viral infection (a Th1 response) and brief allergy exposure-induced lung inflammation (a Th2 response), a clear population of lung-resident antigen-specific CD4 + T cells that is separated from bloodstream forms in an IL-2-dependent manner and play essential functions in local immunity. 180,181 In response to prolonged allergen exposure, a similar CD69 + and Th2-biased CD4 + T RM population persists in the lung parenchyma.…”

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

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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%

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

Section: Cd4+ Trm Cellsmentioning

confidence: 99%

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Tissue-Specific Control of Tissue-Resident Memory T Cells

Liu

Zhang

2018

Crit Rev Immunol

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“…To determine if WT and Fut4/7 −/− OT-II were differentially distributed in the vasculature versus parenchyma lungs, which could potentially account for differences in survival factor usage (29). Thus, WT or Fut4/7 −/− OT-II T cells were co-injected into WT hosts and infected with PR8-OVA II .…”

Section: Resultsmentioning

confidence: 99%

Fucosyltransferase Induction during Influenza Virus Infection Is Required for the Generation of Functional Memory CD4+ T Cells

Tinoco

Carrette

Henriquez

et al. 2018

The Journal of Immunology

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T cells mediating influenza viral control are instructed in lymphoid and nonlymphoid tissues to differentiate into memory T cells that confer protective immunity. The mechanisms by which influenza virus-specific memory CD4+ T cells arise have been attributed to changes in transcription factors, cytokines and cytokine receptors, and metabolic programing. The molecules involved in these biosynthetic pathways including proteins and lipids are modified to varying degrees of glycosylation, fucosylation, sialation, and sulfation, which can alter their function. It is currently unknown how the glycome enzymatic machinery regulates CD4+ T cell effector and memory differentiation. In a murine model of influenza virus infection, we found that fucosyltransferase enzymatic activity was induced in effector and memory CD4+ T cells. Using CD4+ T cells deficient in the Fut4/7 enzymes that are expressed only in hematopoietic cells, we found decreased frequencies of effector cells with reduced expression of T-bet and NKG2A/C/E in the lungs during primary infection. Furthermore, Fut4/7−/− effector CD4+ T cells had reduced survival with no difference in proliferation or capacity for effector function. While Fut4/7−/− CD4+ T cells seeded the memory pool after primary infection, they failed to form tissue resident cells, were dysfunctional and were unable to re-expand after secondary infection. Our findings highlight an important regulatory axis mediated by cell-intrinsic fucosyltransferase activity in CD4+ T cell effectors that ensure the development of functional memory CD4+ T cells.

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“…The lungs contain a population of CD4 + T RM that have been shown to play a critical role in recruiting CD8 + T‐cells and enhancing secondary immune responses against bacterial, viral and worm infections . In an influenza infection model, antigen‐specific memory CD4 + T‐cells migrate to the lungs and are retained in the tissue without recirculation, as demonstrated by parabiosis experiments .…”

Section: Tissue‐resident Cd4+ Memory T‐cellsmentioning

confidence: 99%

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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IL-15 supports the generation of protective lung-resident memory CD4 T cells

Cited by 77 publications

References 53 publications

Tissue-Specific Control of Tissue-Resident Memory T Cells

Tissue-Specific Control of Tissue-Resident Memory T Cells

Fucosyltransferase Induction during Influenza Virus Infection Is Required for the Generation of Functional Memory CD4+ T Cells

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

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IL-15 supports the generation of protective lung-resident memory CD4 T cells

Cited by 77 publications

References 53 publications

Tissue-Specific Control of Tissue-Resident Memory T Cells

Tissue-Specific Control of Tissue-Resident Memory T Cells

Fucosyltransferase Induction during Influenza Virus Infection Is Required for the Generation of Functional Memory CD4+ T Cells

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

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