Deciphering the black box of food allergy mechanisms

Sampath, Vanitha; Tupa, Dana; Graham, Michelle T.; Chatila, Talal A.; Spergel, Jonathan M.; Nadeau, Kari

doi:10.1016/j.anai.2016.10.017

Cited by 25 publications

(21 citation statements)

References 60 publications

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“…Herein, we demonstrate that IL-4 can amplify the IgE-mediated, histamine-induced fluid extravasation through priming of the vascular endothelial compartment. Previous studies have revealed an important role for IL-4 and IL-4Rα signaling in IgE-mediated anaphylaxis; however, this was predominantly thought to be through its effect on the hematopoietic compartment driving IgE-isotype switch and the associated CD4 + Th2 and mast cell response in anaphylaxis 31, 67–69 . We show that IL-4 also acts on the non-hematopoietic compartment, namely the VE to increase the sensitivity of the VE to histamine.…”

Section: Discussionmentioning

confidence: 99%

The vascular endothelial specific IL-4 receptor alpha–ABL1 kinase signaling axis regulates the severity of IgE-mediated anaphylactic reactions

Yamani

Waggoner

et al. 2018

Journal of Allergy and Clinical Immunology

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Background Severe IgE-mediated, food-induced anaphylactic reactions are characterized by pulmonary venous vasodilatation and fluid extravasation, which is thought to lead to the life-threatening anaphylactic phenotype. The underlying immunological and cellular processes involved in driving fluid extravasation and the severe anaphylactic phenotype are not fully elucidated. Objective To define the interaction and requirement of IL-4 and vascular endothelial (VE) IL-4Rα chain signaling in histamine-ABL1–mediated VE dysfunction and fluid extravasation in the severity of IgE-mediated anaphylactic reactions in mice. Methods Mice deficient in VE IL-4Rα and models of passive and active oral antigen– and IgE-induced anaphylaxis were employed to define the requirements of VE IL-4Rα and ABL1 pathway in severe anaphylactic reactions. Human VE cell line (EA.hy926 cells) and pharmacologic (imatinib) and genetic approaches (shRNA knockdown of IL4RA and ABL1) were used to define the requirement of this pathway in VE barrier dysfunction. Results IL-4 exacerbation of histamine-induced hypovolemic shock in mice was dependent on VE expression of the IL-4Rα. IL-4 and histamine induced ABL1 activation in human VE cells and VE barrier dysfunction was ABL1 dependent. Development of severe IgE-mediated hypovolemia and shock required VE-restricted ABL1 expression. Treatment of mice with a history of food-induced anaphylaxis with the ABL kinase inhibitor imatinib protected the mice from developing severe IgE-mediated anaphylaxis. Conclusion IL-4 amplifies IgE- and histamine-induced VE dysfunction, fluid extravasation, and severity of anaphylaxis via a VE IL-4Rα-ABL1–dependent mechanism. These studies implicate an important contribution by the VE compartment in the severity of anaphylaxis and identify a new pathway for therapeutic intervention of IgE-mediated reactions.

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Section: Discussionmentioning

confidence: 99%

The vascular endothelial specific IL-4 receptor alpha–ABL1 kinase signaling axis regulates the severity of IgE-mediated anaphylactic reactions

Yamani

Waggoner

et al. 2018

Journal of Allergy and Clinical Immunology

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“…CX3CR1+ macrophages can capture food antigens directly from the intestinal lumen by insinuating dendritic extensions between epithelial junctions (periscopic mechanism). CD103+ DCs transport the captured antigens to Peyer's patches and mesenteric lymphnodes and drive the homing of B lymphocytes secreting mucosal IgA in the gut, thus contributing to the maintenance of a specific immune tolerance [92]. IgGs, in particular, specific IgG4, can inhibit the initiation as well as the effector phases of allergic responses, thus also contributing to the acquisition of oral tolerance to food antigens [2].…”

Section: Tolerance Disruptionmentioning

confidence: 99%

“…Among the other cell types involved in tolerance disruption, innate lymphoid cells of type 2 (ILC2), similar to Th2 lymphocytes but lacking specificity for the antigen, and IL-9-producing cells (Th9 cells), which are mucosal mastcells capable of producing various inflammatory cytokines and capable to suppress the function of Tregcells, have been recently recognized [2,100]. All of them increase the vicious circle which leads, through an autocrine loop, to the increase in the intestinal mastcell pool [20,92,101].…”

Section: Tolerance Disruptionmentioning

confidence: 99%

New Perspectives in Food Allergy

Martinis

Sirufo

Suppa

et al. 2020

IJMS

175

130

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The improvement of the knowledge of the pathophysiological mechanisms underlying the tolerance and sensitization to food antigens has recently led to a radical change in the clinical approach to food allergies. Epidemiological studies show a global increase in the prevalence of food allergy all over the world and manifestations of food allergy appear increasingly frequent also in elderly subjects. Environmental and nutritional changes have partly changed the epidemiology of allergic reactions to foods and new food allergic syndromes have emerged in recent years. The deepening of the study of the intestinal microbiota has highlighted important mechanisms of immunological adaptation of the mucosal immune system to food antigens, leading to a revolution in the concept of immunological tolerance. As a consequence, new prevention models and innovative therapeutic strategies aimed at a personalized approach to the patient affected by food allergy are emerging. This review focuses on these new perspectives and their practical implications in the management of food allergy, providing an updated view of this complex pathology.

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“…Several Treg subtypes have been associated with tolerance, including Foxp3 + Tregs, IL-10-secreting Foxp3 -Tregs (also known as Tr1 cells), and TGF-β-secreting T helper 3 (Th3) cells. Further details can be found in a number of excellent reviews on the topic (46,48,(62)(63)(64)(65)(66)(67)(68).…”

Section: T Cell Mechanisms Underlying Tolerancementioning

confidence: 99%