From trained immunity in allergy to trained <scp>immunity‐based</scp> allergen vaccines

Martín-Cruz, Leticia; Sevilla-Ortega, Carmen; Angelina, Alba; Domínguez‐Andrés, Jorge; Netea, Mihai G.; Subiza, José Luis; Palomares, Óscar

doi:10.1111/cea.14261

Cited by 9 publications

(11 citation statements)

References 98 publications

(244 reference statements)

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“…Different ventures of existing vaccines or viral components to induce trained immunity seek to improve conventional vaccines toward the new formulations of the so-called trained immunity-based vaccines (TIbV), aimed at stimulating broader responses beyond their specific antigens, an approach that could make it possible to afford proper resistance against viral outbreaks [ 104 , 105 , 106 , 107 ]. However, this might not be the case for allergen vaccines.…”

Section: Trained Immunitymentioning

confidence: 99%

“…However, this might not be the case for allergen vaccines. In a recent study Benito-Villalvilla et al, it was demonstrated that allergoid–mannan conjugates, which serve as next-generation vaccines for allergen-specific immunotherapy (AIT), contribute to allergen tolerance by the differentiation of monocytes into tolerogenic dendritic cells (DCs), but lack the capacity to induce any trained immunity effects [ 107 , 108 ]. Similarly, the innate counterparts of T cells—innate lymphoid cells (ILCs)—primed by IL-33 or allergic inflammation mount enduring memory-like responses against other allergens, which can serve as double-edged sword, on the one side affording proper protection against infectious diseases and, on the other side, by contributing to pathology or disease progression [ 109 , 110 , 111 ].…”

Section: Trained Immunitymentioning

confidence: 99%

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Training vs. Tolerance: The Yin/Yang of the Innate Immune System

et al. 2023

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For almost nearly a century, memory functions have been attributed only to acquired immune cells. Lately, this paradigm has been challenged by an increasing number of studies revealing that innate immune cells are capable of exhibiting memory-like features resulting in increased responsiveness to subsequent challenges, a process known as trained immunity (known also as innate memory). In contrast, the refractory state of endotoxin tolerance has been defined as an immunosuppressive state of myeloid cells portrayed by a significant reduction in the inflammatory capacity. Both training as well tolerance as adaptive features are reported to be accompanied by epigenetic and metabolic alterations occurring in cells. While training conveys proper protection against secondary infections, the induction of endotoxin tolerance promotes repairing mechanisms in the cells. Consequently, the inappropriate induction of these adaptive cues may trigger maladaptive effects, promoting an increased susceptibility to secondary infections—tolerance, or contribute to the progression of the inflammatory disorder—trained immunity. This review aims at the discussion of these opposing manners of innate immune and non-immune cells, describing the molecular, metabolic and epigenetic mechanisms involved and interpreting the clinical implications in various inflammatory pathologies.

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Section: Trained Immunitymentioning

confidence: 99%

Section: Trained Immunitymentioning

confidence: 99%

Training vs. Tolerance: The Yin/Yang of the Innate Immune System

et al. 2023

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“…For example, the presence of stimuli such as dexamethasone (Dex), vitamin D3 (VitD3), rapamycin, or allergoid-mannan conjugates promotes the differentiation of monocytes into tolerogenic DCs or immunosuppressive macrophages ( 22 – 26 ). Conversely, monocytes exposed with whole heat-inactivated Candida albicans or β-glucans from its cell wall give raise to trained monocyte-derived macrophages ( 27 – 29 ). Here, we show that LPS-stimulated WIN-hmoDCs displayed reduced production of the pro-inflammatory cytokines TNFα, IL-1β and IL-6 without changes in IL-10.…”

Section: Discussionmentioning

confidence: 99%

Cannabinoid WIN55,212-2 reprograms monocytes and macrophages to inhibit LPS-induced inflammation

et al. 2023

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IntroductionChronic or uncontrolled activation of myeloid cells including monocytes, macrophages and dendritic cells (DCs) is a hallmark of immune-mediated inflammatory disorders. There is an urgent need for the development of novel drugs with the capacity to impair innate immune cell overactivation under inflammatory conditions. Compelling evidence pointed out cannabinoids as potential therapeutic tools with anti-inflammatory and immunomodulatory capacity. WIN55,212-2, a non-selective synthetic cannabinoid agonist, displays protective effects in several inflammatory conditions by mechanisms partially depending on the generation of tolerogenic DCs able to induce functional regulatory T cells (Tregs). However, its immunomodulatory capacity on other myeloid cells such as monocytes and macrophages remains incompletely understood.MethodsHuman monocyte-derived DCs (hmoDCs) were differentiated in the absence (conventional hmoDCs) or presence of WIN55,212-2 (WIN-hmoDCs). Cells were stimulated with LPS, cocultured with naive T lymphocytes and their cytokine production and ability to induce T cell responses were analysed by ELISA or flow cytometry. To evaluate the effect of WIN55,212-2 in macrophage polarization, human and murine macrophages were activated with LPS or LPS/IFNγ, in the presence or absence of the cannabinoid. Cytokine, costimulatory molecules and inflammasome markers were assayed. Metabolic and chromatin immunoprecipitation assays were also performed. Finally, the protective capacity of WIN55,212-2 was studied in vivo in BALB/c mice after intraperitoneal injection with LPS.ResultsWe show for the first time that the differentiation of hmoDCs in the presence of WIN55,212-2 generates tolerogenic WIN-hmoDCs that are less responsive to LPS stimulation and able to prime Tregs. WIN55,212-2 also impairs the pro-inflammatory polarization of human macrophages by inhibiting cytokine production, inflammasome activation and rescuing macrophages from pyroptotic cell death. Mechanistically, WIN55,212-2 induced a metabolic and epigenetic shift in macrophages by decreasing LPS-induced mTORC1 signaling, commitment to glycolysis and active histone marks in pro-inflammatory cytokine promoters. We confirmed these data in ex vivo LPS-stimulated peritoneal macrophages (PMΦs), which were also supported by the in vivo anti-inflammatory capacity of WIN55,212-2 in a LPS-induced sepsis mouse model.ConclusionOverall, we shed light into the molecular mechanisms by which cannabinoids exert anti-inflammatory properties in myeloid cells, which might well contribute to the future rational design of novel therapeutic strategies for inflammatory disorders.

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“…Postsynaptic reprogramming could be useful during immunization, as innate training confers heterologous protection [68][69][70] from other diseases [71,72] due to the nonspecific trained immunity-based effect of vaccines [73,74]. Indeed, this effect could also increase the efficacy of existing vaccines [75], or bring forth a novel ground-breaking generation of trained immunitybased vaccines to fight infection [76][77][78][79][80] or allergy [81]. The underlying rationale would be that psDC could enhance innate and adaptive responses.…”

Section: Perspectives On the Applications Of Postsynaptic Reprogrammingmentioning

confidence: 99%

Reprogramming dendritic cells through the immunological synapse: A two‐way street

Calzada‐Fraile,

Sánchez‐Madrid

2023

Eur J Immunol

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Dendritic cells (DCs) bridge innate and adaptive immunity. Their main function is to present antigens to prime T cells and initiate and shape adaptive responses. Antigen presentation takes place through intimate contacts between the two cells, termed immune synapses (IS). During formation of IS, information travels towards the T cell side to induce and tune its activation; but it also travels in reverse via engagement of membrane receptors and within extracellular vesicles transferred to the DC. Such reverse information transfer and its consequences on DC fate have been largely neglected. Here, we review the events and effects of IS‐mediated antigen presentation on DCs. In addition, we discuss novel technological advancements that enable monitoring DCs interactions with T lymphocytes, the main effects of DCs undergoing productive IS (post‐synaptic DCs, or psDCs), and how reverse information transfer could be harnessed to modulate immune responses for therapeutic intervention.This article is protected by copyright. All rights reserved

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From trained immunity in allergy to trained immunity‐based allergen vaccines

Cited by 9 publications

References 98 publications

Training vs. Tolerance: The Yin/Yang of the Innate Immune System

Training vs. Tolerance: The Yin/Yang of the Innate Immune System

Cannabinoid WIN55,212-2 reprograms monocytes and macrophages to inhibit LPS-induced inflammation

Reprogramming dendritic cells through the immunological synapse: A two‐way street

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