Transcription Factor IRF8 Orchestrates the Adaptive Natural Killer Cell Response

Adams, Nicholas M.; Lau, Colleen M.; Fan, Xiying; Rapp, Moritz; Geary, Clair D.; Weizman, Orr-El; Díaz-Salazar, Carlos; Sun, Joseph C.

doi:10.1016/j.immuni.2018.04.018

Cited by 102 publications

(101 citation statements)

References 74 publications

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“…This hypothesis was strengthened by the study of Irf8 −/− mice, who were found to have decreased frequency of terminally mature NK cells in peripheral blood and spleen . Further study of these mice showed that they are particularly susceptible to LCMV infection and malignancy and that generation of adaptive NK cells in these mice following infection is impaired . In both murine and human NK cells, IRF8 is up‐regulated in response to cytokine signaling, and in mice, this leads to Stat4‐mediated binding of Irf8 to the cell cycle regulator Zbtb32.…”

Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

“…Further study of these mice showed that they are particularly susceptible to LCMV infection and malignancy and that generation of adaptive NK cells in these mice following infection is impaired . In both murine and human NK cells, IRF8 is up‐regulated in response to cytokine signaling, and in mice, this leads to Stat4‐mediated binding of Irf8 to the cell cycle regulator Zbtb32. In this way, viral infection or expansion in response to tumor challenge leads to Irf8‐mediated NK cell expansion and generation of the NK cell memory pool …”

Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

“…In both murine and human NK cells, IRF8 is up‐regulated in response to cytokine signaling, and in mice, this leads to Stat4‐mediated binding of Irf8 to the cell cycle regulator Zbtb32. In this way, viral infection or expansion in response to tumor challenge leads to Irf8‐mediated NK cell expansion and generation of the NK cell memory pool …”

Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

“…Together, these data suggest that, in both mice and humans, there is a critical link between NK cell development, proliferation, and functional maturation. Given the requirement for IRF8‐driven NK cell expansion, mediated by the cell cycle regulator Zbtb32, in the generation of adaptive NK cells in mice, it is plausible to think that this expansion is the feature that is “broken” in NK cells from patients with CMG complex or biallelic IRF8 mutations. It remains to be seen how this so dramatically affects the function of remaining NK cells in these patients, however, particularly given the presumed retained function of the NK cells in patients with hypomorphic RAG mutations …”

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

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Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Mace

Orange

2018

Immunological Reviews

129

107

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Human NK cells are innate immune effectors that play a critical roles in the control of viral infection and malignancy. The importance of their homeostasis and function can be demonstrated by the study of patients with primary immunodeficiencies (PID), which are part of the family of diseases known as inborn defects of immunity. While NK cells are affected in many PIDs in ways that may contribute to a patient’s clinical phenotype, a small number of PIDs have an NK cell abnormality as their major immunological defect. These PIDs can be collectively referred to as NK cell deficiency disorders (NKD), and include effects upon NK cell numbers, subsets and/or functions. The clinical impact of NKD can be severe including fatal viral infection, with particular susceptibility to herpesviral infections, such as cytomegalovirus, varicella zoster virus and Epstein-Barr virus. While NKD is rare, studies of these diseases are important for defining specific requirements for human NK cell development and homeostasis. New themes in NK cell biology are emerging through the study of both known and novel NKD, particularly those affecting cell cycle and DNA damage repair, as well as broader PIDs having substantive impact upon NK cells. In addition, the discovery of NKD that affect other innate lymphoid cell (ILC) subsets opens new doors for better understanding the relationship between conventional NK cells and other ILC subsets. Here we describe the biology underlying human NKD, particularly in the context of new insights into innate immune cell function, including a discussion of recently described NKD with accompanying effects on ILC subsets. Given the impact of these disorders upon human immunity with a common focus upon NK cells, the unifying message of a critical role for NK cells in human host defense singularly emerges.

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Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

Section: Classical Nkd (Cnkd)mentioning

confidence: 99%

Section: Emerging Themes In Nk Cell Deficiencymentioning

confidence: 99%

See 2 more Smart Citations

Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Mace

Orange

2018

Immunological Reviews

129

107

View full text Add to dashboard Cite

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“…Functionally, STAT4 acts in part by directing a ‘permissive’ chromatin state, likely through the recruitment of histone remodeling enzymes, around target gene loci. Indeed, H3K4 trimethylation at the Runx , Cbfb , and Irf8 promoters was recently shown to occur in a STAT4‐dependent manner during NK cell activation in vitro . The related TF, STAT1 also contributes to the expansion of MCMV‐specific Ly49H + NK cells, acting downstream of type 1 interferon (IFN‐I) signals that serve to protect NK cells from NKG2D‐dependent fratricide .…”

Section: Transcription Factors That Regulate Effector and Memory Nk Cmentioning

confidence: 99%

Transcriptional control of natural killer cell differentiation

Brillantes

Beaulieu

2018

Immunology

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Summary Natural killer (NK) cells are highly specialized cytotoxic lymphocytes that provide protection against pathogens and malignant cells. They develop from common lymphoid progenitors via a multi‐stage lineage commitment and differentiation process that gives rise to mature NK cells with potent cytotoxic functionality. Although generally considered cells of the innate immune system, recent studies have demonstrated that NK cells have the capacity to mount immune responses with features of adaptive immunity, including robust antigen‐specific clonal‐like expansion and the generation of long‐lived memory cells that mediate enhanced recall responses. Here, we discuss specific transcription factors that have been shown to commonly and uniquely regulate NK cell development and effector and memory responses in experimental mouse models.

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IRF8 Impacts Self‐Renewal of Hematopoietic Stem Cells by Regulating TLR9 Signaling Pathway of Innate Immune Cells

Zhang

Qiu

et al. 2021

Advanced Science

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IRF8 is a key regulator of innate immunity receptor signaling and plays diverse functions in the development of hematopoietic cells. The effects of IRF8 on hematopoietic stem cells (HSCs) are still unknown. Here, it is demonstrated that IRF8 deficiency results in a decreased number of long-term HSCs (LT-HSCs) in mice. However, the repopulation capacity of individual HSCs is significantly increased. Transcriptomic analysis shows that IFN-and IFNsignaling is downregulated in IRF8-deficient HSCs, while their response to proinflammatory cytokines is unchanged ex vivo. Further tests show that Irf8 −/− HSCs can not respond to CpG, an agonist of Toll-like receptor 9 (TLR9) in mice, while long-term CpG stimulation increases wild-type HSC abundance and decreases their bone marrow colony-forming capacity. Mechanistically, as the primary producer of proinflammatory cytokines in response to CpG stimulation, dendritic cells has a blocked TLR9 signaling due to developmental defect in Irf8 −/− mice. Macrophages remain functionally intact but severely reduce in Irf8 −/− mice. In NK cells, IRF8 directly regulates the expression of Tlr9 and its deficiency leads to no increased IFN production upon CpG stimulation. These results indicate that IRF8 regulates HSCs, at least in part, through controlling TLR9 signaling in diverse innate immune cells.

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Transcription Factor IRF8 Orchestrates the Adaptive Natural Killer Cell Response

Cited by 102 publications

References 74 publications

Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Emerging insights into human health and NK cell biology from the study of NK cell deficiencies

Transcriptional control of natural killer cell differentiation

IRF8 Impacts Self‐Renewal of Hematopoietic Stem Cells by Regulating TLR9 Signaling Pathway of Innate Immune Cells

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