Bruton’s tyrosine kinase inhibition effectively protects against human IgE-mediated anaphylaxis
Melanie C. Dispenza, … , Piper A. Robida, Bruce S. Bochner
Melanie C. Dispenza, … , Piper A. Robida, Bruce S. Bochner
Published June 2, 2020
Citation Information: J Clin Invest. 2020;130(9):4759-4770. https://doi.org/10.1172/JCI138448.
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Bruton’s tyrosine kinase inhibition effectively protects against human IgE-mediated anaphylaxis

Abstract

No known therapies can prevent anaphylaxis. Bruton’s tyrosine kinase (BTK) is an enzyme thought to be essential for high-affinity IgE receptor (FcεRI) signaling in human cells. We tested the hypothesis that FDA-approved BTK inhibitors (BTKis) would prevent IgE-mediated responses including anaphylaxis. We showed that irreversible BTKis broadly prevented IgE-mediated degranulation and cytokine production in primary human mast cells and blocked allergen-induced contraction of isolated human bronchi. To address their efficacy in vivo, we created and used what we believe to be a novel humanized mouse model of anaphylaxis that does not require marrow ablation or human tissue implantation. After a single intravenous injection of human CD34+ cells, NSG-SGM3 mice supported the population of mature human tissue-resident mast cells and basophils. These mice showed excellent responses during passive systemic anaphylaxis using human IgE to selectively evoke human mast cell and basophil activation, and response severity was controllable by alteration of the amount of allergen used for challenge. Remarkably, pretreatment with just 2 oral doses of the BTKi acalabrutinib completely prevented moderate IgE-mediated anaphylaxis in these mice and also significantly protected against death during severe anaphylaxis. Our data suggest that BTKis may be able to prevent anaphylaxis in humans by inhibiting FcεRI-mediated signaling.

Authors

Melanie C. Dispenza, Rebecca A. Krier-Burris, Krishan D. Chhiba, Bradley J. Undem, Piper A. Robida, Bruce S. Bochner

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Figure 2

Ibrutinib effectively blocks anti-IgE–induced contraction of human bronchi.

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Ibrutinib effectively blocks anti-IgE–induced contraction of human bronc...
Isolated human bronchi were pretreated with ibrutinib or vehicle for 30 minutes, and then anti-IgE–induced contraction was measured. (A) Cumulative concentration-response curves for anti-IgE–induced contractions are shown for vehicle- and ibrutinib-treated tissues. Contraction is expressed as a percentage of the maximal obtainable contraction evoked by carbamylcholine (100 μM) added at the end of the experiment. n = 4 using bronchi from different donors. (B) Percentage of maximal contraction as achieved by treatment with exogenous histamine is shown for tissues treated with vehicle or 1 μM ibrutinib. n = 2 from different donors. All data are displayed as means ± SEM. ****P < 0.0001 compared with vehicle-treated tissues by 2-way ANOVA with repeated measures. NS, not significant by 2-tailed paired Student’s t test.