Type I, II, and III Interferons: Regulating Immunity to Mycobacterium tuberculosis Infection

Travar, Maja; Petković, Miroslav; Verhaz, Antonija

doi:10.1007/s00005-015-0365-7

Cited by 35 publications

(35 citation statements)

References 112 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…and are considered critical to obtain effective anti-tumor T cell responses. Interferons (IFNs) represent a large group of cytokines, typically divided among type I (generally IFN-α,β) II (IFN-γ) and III (IFN-λ) [33]. Pro-inflammatory cytokines, excreted from inflammation-promoting immune cells, such as macrophages and helper T cells, include interleukins-1 (IL-1), 6, 8, 12, 18, 21, GM-CSF, and TNF-α.…”

Section: Article Highlightsmentioning

confidence: 99%

Consumption of β-glucans to spice up T cell treatment of tumors: a review

Graaff

Govers

Wichers

et al. 2018

Expert Opinion on Biological Therapy

View full text Add to dashboard Cite

Adoptive T-cell treatments of solid cancers have evolved into a robust therapy with objective response rates surpassing those of standardized treatments. Unfortunately, only a limited fraction of patients shows durable responses, which is considered to be due to a T cell-suppressive tumor microenvironment (TME). Here we argue that naturally occurring β-glucans can enable reversion of such T cell suppression by engaging innate immune cells and enhancing numbers and function of lymphocyte effectors. Areas covered: This review summarizes timely reports with respect to absorption, trafficking and immune stimulatory effects of β-glucans, particularly in relation to innate immune cells. Furthermore, we list effects toward well-being and immune functions in healthy subjects as well as cancer patients treated with orally administered β-glucans, extended with effects of β-glucan treatments in mouse cancer models. Expert opinion: Beta-glucans, when present in food and following uptake in the proximal gut, stimulate immune cells present in gut-associated lymphoid tissue and initiate highly conserved pro-inflammatory pathways. When tested in mouse cancer models, β-glucans result in better control of tumor growth and shift the TME toward a T cell-sensitive environment. Along these lines, we advocate that intake of β-glucans provides an accessible and immune-potentiating adjuvant when combined with adoptive T-cell treatments of cancer.

show abstract

Section: Article Highlightsmentioning

confidence: 99%

Consumption of β-glucans to spice up T cell treatment of tumors: a review

Graaff

Govers

Wichers

et al. 2018

Expert Opinion on Biological Therapy

View full text Add to dashboard Cite

show abstract

“…The production of IFN-gamma by immune cells is an essential defense mechanism against many viral, bacterial, and parasitic infections (Borges da Silva et al, 2015 ). NK cells are a major innate source of IFN-gamma (Travar et al, 2016 ; Waggoner et al, 2016 ). Although CD4 + T cells are a major adaptive source of IFN-gamma, their ability to respond to infection is slower than that of NK cells.…”

Section: Car-modified Nk Cell-based Immunotherapy To Treat Infectiousmentioning

confidence: 99%

Chimeric antigen receptor (CAR)-modified natural killer cell-based immunotherapy and immunological synapse formation in cancer and HIV

et al. 2017

View full text Add to dashboard Cite

Cytotoxic T lymphocytes (CTLs) and natural killer (NK) cells contribute to the body’s immune defenses. Current chimeric antigen receptor (CAR)-modified T cell immunotherapy shows strong promise for treating various cancers and infectious diseases. Although CAR-modified NK cell immunotherapy is rapidly gaining attention, its clinical applications are mainly focused on preclinical investigations using the NK92 cell line. Despite recent advances in CAR-modified T cell immunotherapy, cost and severe toxicity have hindered its widespread use. To alleviate these disadvantages of CAR-modified T cell immunotherapy, additional cytotoxic cell-mediated immunotherapies are urgently needed. The unique biology of NK cells allows them to serve as a safe, effective, alternative immunotherapeutic strategy to CAR-modified T cells in the clinic. While the fundamental mechanisms underlying the cytotoxicity and side effects of CAR-modified T and NK cell immunotherapies remain poorly understood, the formation of the immunological synapse (IS) between CAR-modified T or NK cells and their susceptible target cells is known to be essential. The role of the IS in CAR T and NK cell immunotherapies will allow scientists to harness the power of CAR-modified T and NK cells to treat cancer and infectious diseases. In this review, we highlight the potential applications of CAR-modified NK cells to treat cancer and human immunodeficiency virus (HIV), and discuss the challenges and possible future directions of CAR-modified NK cell immunotherapy, as well as the importance of understanding the molecular mechanisms of CAR-modified T cell- or NK cell-mediated cytotoxicity and side effects, with a focus on the CAR-modified NK cell IS.

show abstract

“…TLR6 diversity (Fig. 2) and age group in Released by CD4 and CD8 cells after infection, IFNγ is a potent immune mediator, activating the immune 233 system in response to mycobacterial antigens (Travar et al, 2016). Animals with a strong IFNγ release 234 following PPD exposure were better able to restrict mycobacterial growth in the whole blood assay, 235 supporting the role of this gene in the innate immune response to mycobacteria.…”

Section: Predictors Of Mycobacterial Growth 203mentioning

confidence: 91%