Literature DB >> 33715245

Pathogenesis of IgE-mediated food allergy and implications for future immunotherapeutics.

Nicole Ramsey1, M Cecilia Berin1.   

Abstract

Our understanding of the immune basis of food allergy has grown rapidly in parallel with the development of new immune-targeted interventions for the treatment of food allergy. Local tissue factors, including the composition of skin and gastrointestinal microbiota and production of Th2-inducing cytokines (TSLP, IL-33, and IL-25) from barrier sites, have been shown not only to contribute to the development of food allergy, but also to act as effective targets for treatment in mice. Ongoing clinical trials are testing the targeting of these factors in human disease. There is a growing understanding of the contribution of IL-13 to the induction of high-affinity IgE and the need for continual T-cell help in the maintenance of long-lived IgE. This provides a strong rationale to test biologics targeting both IL-4 and IL-13 in the treatment of established food allergy. Various forms of allergen immunotherapy for food allergy have clearly shown that low specific IgE and elevated specific IgG4 are predictive of sustained treatment effect. Treatments that mimic that immune response, for example, lowering IgE, with monoclonal antibodies such as omalizumab, or administering allergen-specific IgG, are in various stages of investigation. As we gain more opportunities to use immune-modifying treatments for the treatment of food allergy, studies of the immune and clinical response to those interventions will continue to rapidly advance our understanding of the immune basis of food allergy and tolerance.
© 2021 European Academy of Allergy and Clinical Immunology and John Wiley & Sons Ltd.

Entities:  

Keywords:  IgE; IgG4; Tfh13; Th2; Th2a; epicutaneous immunotherapy; food immunotherapy; oral immunotherapy; regulatory T cell; sublingual immunotherapy

Mesh:

Substances:

Year:  2021        PMID: 33715245      PMCID: PMC9096874          DOI: 10.1111/pai.13501

Source DB:  PubMed          Journal:  Pediatr Allergy Immunol        ISSN: 0905-6157            Impact factor:   5.464


  63 in total

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5.  Sustained outcomes in oral immunotherapy for peanut allergy (POISED study): a large, randomised, double-blind, placebo-controlled, phase 2 study.

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Journal:  J Allergy Clin Immunol       Date:  2015-11-12       Impact factor: 10.793

7.  The nonlesional skin surface distinguishes atopic dermatitis with food allergy as a unique endotype.

Authors:  Donald Y M Leung; Agustin Calatroni; Livia S Zaramela; Petra K LeBeau; Nathan Dyjack; Kanwaljit Brar; Gloria David; Keli Johnson; Susan Leung; Marco Ramirez-Gama; Bo Liang; Cydney Rios; Michael T Montgomery; Brittany N Richers; Clifton F Hall; Kathryn A Norquest; John Jung; Irina Bronova; Simion Kreimer; C Conover Talbot; Debra Crumrine; Robert N Cole; Peter Elias; Karsten Zengler; Max A Seibold; Evgeny Berdyshev; Elena Goleva
Journal:  Sci Transl Med       Date:  2019-02-20       Impact factor: 17.956

8.  Observational long-term follow-up study of rapid food oral immunotherapy with omalizumab.

Authors:  Sandra Andorf; Monali Manohar; R Sharon Chinthrajah; Kari C Nadeau; Tina Dominguez; Whitney Block; Dana Tupa; Rohun A Kshirsagar; Vanitha Sampath
Journal:  Allergy Asthma Clin Immunol       Date:  2017-12-21       Impact factor: 3.406

9.  Origins and clonal convergence of gastrointestinal IgE+ B cells in human peanut allergy.

Authors:  Ramona A Hoh; Shilpa A Joshi; Ji-Yeun Lee; Brock A Martin; Sushama Varma; Shirley Kwok; Sandra C A Nielsen; Parastu Nejad; Emily Haraguchi; Priya S Dixit; Swetha V Shutthanandan; Krishna M Roskin; Wenming Zhang; Dana Tupa; Bryan J Bunning; Monali Manohar; Robert Tibshirani; Nielsen Q Fernandez-Becker; Neeraja Kambham; Robert B West; Robert G Hamilton; Mindy Tsai; Stephen J Galli; Rebecca S Chinthrajah; Kari C Nadeau; Scott D Boyd
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Review 10.  Filaggrin gene defects and risk of developing allergic sensitisation and allergic disorders: systematic review and meta-analysis.

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  1 in total

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