A γδ T cell–IL-3 axis controls allergic responses through sensory neurons

Cameron H. Flayer; Isabela J. Kernin; Peri R. Matatia; Xiangsunze Zeng; David A. Yarmolinsky; Cai Han; Parth R. Naik; Dean R. Buttaci; Pamela A. Aderhold; Ryan B. Camire; Xueping Zhu; Alice J. Tirard; John T. McGuire; Neal P. Smith; Clive S. McKimmie; Cameron S. McAlpine; Filip K. Swirski; Clifford J. Woolf; Alexandra Chloe Villani; Caroline L. Sokol

doi:10.1038/s41586-024-07869-0

A γδ T cell–IL-3 axis controls allergic responses through sensory neurons

Cameron H. Flayer, Isabela J. Kernin, Peri R. Matatia, Xiangsunze Zeng, David A. Yarmolinsky, Cai Han, Parth R. Naik, Dean R. Buttaci, Pamela A. Aderhold, Ryan B. Camire, Xueping Zhu, Alice J. Tirard, John T. McGuire, Neal P. Smith, Clive S. McKimmie, Cameron S. McAlpine, Filip K. Swirski, Clifford J. Woolf, Alexandra Chloe Villani, Caroline L. Sokol

Research output: Contribution to journal › Article › peer-review

19 Scopus citations

Abstract

In naive individuals, sensory neurons directly detect and respond to allergens, leading to both the sensation of itch and the activation of local innate immune cells, which initiate the allergic immune response^1,2. In the setting of chronic allergic inflammation, immune factors prime sensory neurons, causing pathologic itch^3–7. Although these bidirectional neuroimmune circuits drive responses to allergens, whether immune cells regulate the set-point for neuronal activation by allergens in the naive state is unknown. Here we describe a γδ T cell–IL-3 signalling axis that controls the allergen responsiveness of cutaneous sensory neurons. We define a poorly characterized epidermal γδ T cell subset⁸, termed GD3 cells, that produces its hallmark cytokine IL-3 to promote allergic itch and the initiation of the allergic immune response. Mechanistically, IL-3 acts on Il3ra-expressing sensory neurons in a JAK2-dependent manner to lower their threshold for allergen activation without independently eliciting itch. This γδ T cell–IL-3 signalling axis further acts by means of STAT5 to promote neuropeptide production and the initiation of allergic immunity. These results reveal an endogenous immune rheostat that sits upstream of and governs sensory neuronal responses to allergens on first exposure. This pathway may explain individual differences in allergic susceptibility and opens new therapeutic avenues for treating allergic diseases.

Original language	English
Pages (from-to)	440-446
Number of pages	7
Journal	Nature
Volume	634
Issue number	8033
DOIs	https://doi.org/10.1038/s41586-024-07869-0
State	Published - 10 Oct 2024

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Flayer, C. H., Kernin, I. J., Matatia, P. R., Zeng, X., Yarmolinsky, D. A., Han, C., Naik, P. R., Buttaci, D. R., Aderhold, P. A., Camire, R. B., Zhu, X., Tirard, A. J., McGuire, J. T., Smith, N. P., McKimmie, C. S., McAlpine, C. S., Swirski, F. K., Woolf, C. J., Villani, A. C., & Sokol, C. L. (2024). A γδ T cell–IL-3 axis controls allergic responses through sensory neurons. Nature, 634(8033), 440-446. https://doi.org/10.1038/s41586-024-07869-0

@article{55c5abe0f5df4202b234a9d12f5858b3,

title = "A γδ T cell–IL-3 axis controls allergic responses through sensory neurons",

abstract = "In naive individuals, sensory neurons directly detect and respond to allergens, leading to both the sensation of itch and the activation of local innate immune cells, which initiate the allergic immune response1,2. In the setting of chronic allergic inflammation, immune factors prime sensory neurons, causing pathologic itch3–7. Although these bidirectional neuroimmune circuits drive responses to allergens, whether immune cells regulate the set-point for neuronal activation by allergens in the naive state is unknown. Here we describe a γδ T cell–IL-3 signalling axis that controls the allergen responsiveness of cutaneous sensory neurons. We define a poorly characterized epidermal γδ T cell subset8, termed GD3 cells, that produces its hallmark cytokine IL-3 to promote allergic itch and the initiation of the allergic immune response. Mechanistically, IL-3 acts on Il3ra-expressing sensory neurons in a JAK2-dependent manner to lower their threshold for allergen activation without independently eliciting itch. This γδ T cell–IL-3 signalling axis further acts by means of STAT5 to promote neuropeptide production and the initiation of allergic immunity. These results reveal an endogenous immune rheostat that sits upstream of and governs sensory neuronal responses to allergens on first exposure. This pathway may explain individual differences in allergic susceptibility and opens new therapeutic avenues for treating allergic diseases.",

author = "Flayer, \{Cameron H.\} and Kernin, \{Isabela J.\} and Matatia, \{Peri R.\} and Xiangsunze Zeng and Yarmolinsky, \{David A.\} and Cai Han and Naik, \{Parth R.\} and Buttaci, \{Dean R.\} and Aderhold, \{Pamela A.\} and Camire, \{Ryan B.\} and Xueping Zhu and Tirard, \{Alice J.\} and McGuire, \{John T.\} and Smith, \{Neal P.\} and McKimmie, \{Clive S.\} and McAlpine, \{Cameron S.\} and Swirski, \{Filip K.\} and Woolf, \{Clifford J.\} and Villani, \{Alexandra Chloe\} and Sokol, \{Caroline L.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature Limited 2024.",

year = "2024",

month = oct,

day = "10",

doi = "10.1038/s41586-024-07869-0",

language = "English",

volume = "634",

pages = "440--446",

journal = "Nature",

issn = "0028-0836",

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Flayer, CH, Kernin, IJ, Matatia, PR, Zeng, X, Yarmolinsky, DA, Han, C, Naik, PR, Buttaci, DR, Aderhold, PA, Camire, RB, Zhu, X, Tirard, AJ, McGuire, JT, Smith, NP, McKimmie, CS, McAlpine, CS , Swirski, FK, Woolf, CJ, Villani, AC & Sokol, CL 2024, 'A γδ T cell–IL-3 axis controls allergic responses through sensory neurons', Nature, vol. 634, no. 8033, pp. 440-446. https://doi.org/10.1038/s41586-024-07869-0

TY - JOUR

T1 - A γδ T cell–IL-3 axis controls allergic responses through sensory neurons

AU - Flayer, Cameron H.

AU - Kernin, Isabela J.

AU - Matatia, Peri R.

AU - Zeng, Xiangsunze

AU - Yarmolinsky, David A.

AU - Han, Cai

AU - Naik, Parth R.

AU - Buttaci, Dean R.

AU - Aderhold, Pamela A.

AU - Camire, Ryan B.

AU - Zhu, Xueping

AU - Tirard, Alice J.

AU - McGuire, John T.

AU - Smith, Neal P.

AU - McKimmie, Clive S.

AU - McAlpine, Cameron S.

AU - Swirski, Filip K.

AU - Woolf, Clifford J.

AU - Villani, Alexandra Chloe

AU - Sokol, Caroline L.

PY - 2024/10/10

Y1 - 2024/10/10

N2 - In naive individuals, sensory neurons directly detect and respond to allergens, leading to both the sensation of itch and the activation of local innate immune cells, which initiate the allergic immune response1,2. In the setting of chronic allergic inflammation, immune factors prime sensory neurons, causing pathologic itch3–7. Although these bidirectional neuroimmune circuits drive responses to allergens, whether immune cells regulate the set-point for neuronal activation by allergens in the naive state is unknown. Here we describe a γδ T cell–IL-3 signalling axis that controls the allergen responsiveness of cutaneous sensory neurons. We define a poorly characterized epidermal γδ T cell subset8, termed GD3 cells, that produces its hallmark cytokine IL-3 to promote allergic itch and the initiation of the allergic immune response. Mechanistically, IL-3 acts on Il3ra-expressing sensory neurons in a JAK2-dependent manner to lower their threshold for allergen activation without independently eliciting itch. This γδ T cell–IL-3 signalling axis further acts by means of STAT5 to promote neuropeptide production and the initiation of allergic immunity. These results reveal an endogenous immune rheostat that sits upstream of and governs sensory neuronal responses to allergens on first exposure. This pathway may explain individual differences in allergic susceptibility and opens new therapeutic avenues for treating allergic diseases.

AB - In naive individuals, sensory neurons directly detect and respond to allergens, leading to both the sensation of itch and the activation of local innate immune cells, which initiate the allergic immune response1,2. In the setting of chronic allergic inflammation, immune factors prime sensory neurons, causing pathologic itch3–7. Although these bidirectional neuroimmune circuits drive responses to allergens, whether immune cells regulate the set-point for neuronal activation by allergens in the naive state is unknown. Here we describe a γδ T cell–IL-3 signalling axis that controls the allergen responsiveness of cutaneous sensory neurons. We define a poorly characterized epidermal γδ T cell subset8, termed GD3 cells, that produces its hallmark cytokine IL-3 to promote allergic itch and the initiation of the allergic immune response. Mechanistically, IL-3 acts on Il3ra-expressing sensory neurons in a JAK2-dependent manner to lower their threshold for allergen activation without independently eliciting itch. This γδ T cell–IL-3 signalling axis further acts by means of STAT5 to promote neuropeptide production and the initiation of allergic immunity. These results reveal an endogenous immune rheostat that sits upstream of and governs sensory neuronal responses to allergens on first exposure. This pathway may explain individual differences in allergic susceptibility and opens new therapeutic avenues for treating allergic diseases.

UR - https://www.scopus.com/pages/publications/85203138099

U2 - 10.1038/s41586-024-07869-0

DO - 10.1038/s41586-024-07869-0

M3 - Article

AN - SCOPUS:85203138099

SN - 0028-0836

VL - 634

SP - 440

EP - 446

JO - Nature

JF - Nature

IS - 8033

ER -

A γδ T cell–IL-3 axis controls allergic responses through sensory neurons

Abstract

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