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Citations to this article

Peanut oral immunotherapy differentially suppresses clonally distinct subsets of T helper cells
Brinda Monian, … , Wayne G. Shreffler, J. Christopher Love
Brinda Monian, … , Wayne G. Shreffler, J. Christopher Love
Published November 23, 2021
Citation Information: J Clin Invest. 2022;132(2):e150634. https://doi.org/10.1172/JCI150634.
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Research Article Immunology Article has an altmetric score of 4

Peanut oral immunotherapy differentially suppresses clonally distinct subsets of T helper cells

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Abstract

Food allergy affects an estimated 8% of children in the United States. Oral immunotherapy (OIT) is a recently approved treatment, with outcomes ranging from sustained tolerance to food allergens to no apparent benefit. The immunological underpinnings that influence clinical outcomes of OIT remain largely unresolved. Using single-cell RNA-Seq and paired T cell receptor α/β (TCRα/β) sequencing, we assessed the transcriptomes of CD154+ and CD137+ peanut-reactive T helper (Th) cells from 12 patients with peanut allergy longitudinally throughout OIT. We observed expanded populations of cells expressing Th1, Th2, and Th17 signatures that further separated into 6 clonally distinct subsets. Four of these subsets demonstrated a convergence of TCR sequences, suggesting antigen-driven T cell fates. Over the course of OIT, we observed suppression of Th2 and Th1 gene signatures in effector clonotypes but not T follicular helper–like (Tfh-like) clonotypes. Positive outcomes were associated with stronger suppression of Th2 signatures in Th2A-like cells, while treatment failure was associated with the expression of baseline inflammatory gene signatures that were present in Th1 and Th17 cell populations and unmodulated by OIT. These results demonstrate that differential clinical responses to OIT are associated with both preexisting characteristics of peanut-reactive CD4+ T cells and suppression of a subset of Th2 cells.

Authors

Brinda Monian, Ang A. Tu, Bert Ruiter, Duncan M. Morgan, Patrick M. Petrossian, Neal P. Smith, Todd M. Gierahn, Julia H. Ginder, Wayne G. Shreffler, J. Christopher Love

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Total citations by year

Year: 2025 2024 2023 2022 Total
Citations: 6 11 18 10 45
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Citations to this article (45)

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Nature Communications 2025
New insights into the mechanisms of childhood food allergies
Gubbels L, Saffery R, Neeland MR
Pediatric Allergy and Immunology 2025
A phenotypically distinct human Th2 cell subpopulation is associated with development of allergic disorders in infancy
Pizzarello CR, Jackson CM, Herman K, Seppo AE, Rebhahn J, Scherzi T, Berin MC, Looney RJ, Mosmann TR, Jӓrvinen KM
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Food Allergen Immunotherapy in the Treatment of Patients with IgE-Mediated Food Allergy
Turkalj M, Miletić Gospić A, Višekruna Džidić I, Banić I
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Clinical and experimental allergy : journal of the British Society for Allergy and Clinical Immunology 2024
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Saito A, Koya T, Aoki A, Naramoto S, Ueno H, Nishiyama Y, Shima K, Kimura Y, Hasegawa T, Watanabe S, Ohshima Y, Suzuki K, Ohashi-Doi K, Kikuchi T
Scientific reports 2024
Role of allergen immunotherapy and biologics in allergic diseases
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Current opinion in immunology 2024
Immunomodulatory metabolites in IgE-mediated food allergy and oral immunotherapy outcomes based on metabolomic profiling
Virkud YV, Styles JN, Kelly RS, Patil SU, Ruiter B, Smith NP, Clish C, Wheelock CE, Celedón JC, Litonjua AA, Bunyavanich S, Weiss ST, Baker ES, Lasky-Su JA, Shreffler WG
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Differential Tfh cell phenotypes distinguish IgE-mediated milk allergy from eosinophilic esophagitis in children
Lozano-Ojalvo D, Chen X, Kazmi W, Menchén-Martínez D, Pérez-Rodríguez L, Fernandes-Braga W, Tyler S, Benkov K, Pittman N, Lai J, Sampson HA, de Lafaille MC, Dunkin D, Cecilia Berin M
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Nature reviews. Drug discovery 2024
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Immunological reviews 2024
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Journal of Clinical Investigation 2023
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Current Opinion in Immunology 2023
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Ahlberg E, Al-Kaabawi A, Thune R, Simpson MR, Pedersen SA, Cione E, Jenmalm MC, Tingö L
Frontiers in immunology 2023
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Frontiers in immunology 2023
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The World Allergy Organization journal 2023
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