Peripheral immune-inducer dendritic cells drive early-life allergic inflammation

Yue Xing; Ilana Reznikov; Abonti Nur Ahmed; Ikjot Sidhu; Jill Wisnewski; Asma Farhat; Aleksandr Prystupa; Piotr Konieczny; Kody Mansfield; Melissa L. Cooper; Stephen T. Yeung; Madeline Kim; Sophia Adeghe; Katherine D. Gaines; Meredith Manson; Ji Hyun Sim; Qingrong Huang; Ata S. Moshiri; Kamal M. Khanna; Theresa T. Lu; Emma Guttman-Yassky; Amanda W. Lund; Niroshana Anandasabapathy; Shruti Naik

doi:10.1038/s41586-026-10162-x

Peripheral immune-inducer dendritic cells drive early-life allergic inflammation

Yue Xing
, Ilana Reznikov
, Abonti Nur Ahmed
, Ikjot Sidhu
, Jill Wisnewski
, Asma Farhat
, Aleksandr Prystupa
, Piotr Konieczny
, Kody Mansfield
, Melissa L. Cooper
, Stephen T. Yeung
, Madeline Kim
, Sophia Adeghe
, Katherine D. Gaines
, Meredith Manson
, Ji Hyun Sim
, Qingrong Huang
, Ata S. Moshiri
, Kamal M. Khanna
, Theresa T. Lu

Emma Guttman-Yassky, Amanda W. Lund, Niroshana Anandasabapathy, Shruti Naik

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

1 Scopus citations

Abstract

Atopic diseases associated with allergens, as well as allergic diseases, frequently arise early in life; however, the age-dependent mechanisms governing immune responses to allergens remain poorly understood¹. Here we find that in early life, exposure to common allergens triggers a distinct bifurcated immune response, simultaneously triggering type 17 inflammation in the skin and initiating canonical T helper 2 sensitization in the lymph nodes. This early-life γδ type 17-mediated dermatitis primes the exaggerated allergic lung inflammation upon secondary allergen exposure. Mechanistically, we find dendritic cell (DC)-mediated type 17 activation directly in the skin without requiring migration to lymph nodes; we term this state ‘peripheral immune inducer’ (pii) DC. CD301b⁺ conventional type 2 DCs acquire allergen, adopt the pii-DC state, produce IL-23 and activate local γδ type 17 cells independently of lymph-node engagement. The pii-DC state is enabled by the immature hypothalamic–pituitary–adrenal axis and physiologically low systemic glucocorticoids characteristic of early life^2,3; DC-specific deletion of the glucocorticoid receptor recapitulates the pii-DC phenotype. These findings define a developmental checkpoint, set by neuroendocrine maturation, that enables in situ DC activation and immune induction, thereby shaping age-dependent responses to allergens.

Original language	English
Pages (from-to)	1308-1317
Number of pages	10
Journal	Nature
Volume	652
Issue number	8112
DOIs	https://doi.org/10.1038/s41586-026-10162-x
State	Published - 30 Apr 2026

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Xing, Y., Reznikov, I., Ahmed, A. N., Sidhu, I., Wisnewski, J., Farhat, A., Prystupa, A., Konieczny, P., Mansfield, K., Cooper, M. L., Yeung, S. T., Kim, M., Adeghe, S., Gaines, K. D., Manson, M., Sim, J. H., Huang, Q., Moshiri, A. S., Khanna, K. M., ... Naik, S. (2026). Peripheral immune-inducer dendritic cells drive early-life allergic inflammation. Nature, 652(8112), 1308-1317. https://doi.org/10.1038/s41586-026-10162-x

@article{d3aeac30ccc54ad8893e3a0ded780cda,

title = "Peripheral immune-inducer dendritic cells drive early-life allergic inflammation",

abstract = "Atopic diseases associated with allergens, as well as allergic diseases, frequently arise early in life; however, the age-dependent mechanisms governing immune responses to allergens remain poorly understood1. Here we find that in early life, exposure to common allergens triggers a distinct bifurcated immune response, simultaneously triggering type 17 inflammation in the skin and initiating canonical T helper 2 sensitization in the lymph nodes. This early-life γδ type 17-mediated dermatitis primes the exaggerated allergic lung inflammation upon secondary allergen exposure. Mechanistically, we find dendritic cell (DC)-mediated type 17 activation directly in the skin without requiring migration to lymph nodes; we term this state {\textquoteleft}peripheral immune inducer{\textquoteright} (pii) DC. CD301b+ conventional type 2 DCs acquire allergen, adopt the pii-DC state, produce IL-23 and activate local γδ type 17 cells independently of lymph-node engagement. The pii-DC state is enabled by the immature hypothalamic–pituitary–adrenal axis and physiologically low systemic glucocorticoids characteristic of early life2,3; DC-specific deletion of the glucocorticoid receptor recapitulates the pii-DC phenotype. These findings define a developmental checkpoint, set by neuroendocrine maturation, that enables in situ DC activation and immune induction, thereby shaping age-dependent responses to allergens.",

author = "Yue Xing and Ilana Reznikov and Ahmed, \{Abonti Nur\} and Ikjot Sidhu and Jill Wisnewski and Asma Farhat and Aleksandr Prystupa and Piotr Konieczny and Kody Mansfield and Cooper, \{Melissa L.\} and Yeung, \{Stephen T.\} and Madeline Kim and Sophia Adeghe and Gaines, \{Katherine D.\} and Meredith Manson and Sim, \{Ji Hyun\} and Qingrong Huang and Moshiri, \{Ata S.\} and Khanna, \{Kamal M.\} and Lu, \{Theresa T.\} and Emma Guttman-Yassky and Lund, \{Amanda W.\} and Niroshana Anandasabapathy and Shruti Naik",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature Limited 2026.",

year = "2026",

month = apr,

day = "30",

doi = "10.1038/s41586-026-10162-x",

language = "English",

volume = "652",

pages = "1308--1317",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Research",

number = "8112",

}

Xing, Y, Reznikov, I, Ahmed, AN, Sidhu, I, Wisnewski, J, Farhat, A, Prystupa, A, Konieczny, P, Mansfield, K, Cooper, ML, Yeung, ST, Kim, M, Adeghe, S, Gaines, KD, Manson, M, Sim, JH, Huang, Q, Moshiri, AS, Khanna, KM, Lu, TT, Guttman-Yassky, E, Lund, AW, Anandasabapathy, N & Naik, S 2026, 'Peripheral immune-inducer dendritic cells drive early-life allergic inflammation', Nature, vol. 652, no. 8112, pp. 1308-1317. https://doi.org/10.1038/s41586-026-10162-x

TY - JOUR

T1 - Peripheral immune-inducer dendritic cells drive early-life allergic inflammation

AU - Xing, Yue

AU - Reznikov, Ilana

AU - Ahmed, Abonti Nur

AU - Sidhu, Ikjot

AU - Wisnewski, Jill

AU - Farhat, Asma

AU - Prystupa, Aleksandr

AU - Konieczny, Piotr

AU - Mansfield, Kody

AU - Cooper, Melissa L.

AU - Yeung, Stephen T.

AU - Kim, Madeline

AU - Adeghe, Sophia

AU - Gaines, Katherine D.

AU - Manson, Meredith

AU - Sim, Ji Hyun

AU - Huang, Qingrong

AU - Moshiri, Ata S.

AU - Khanna, Kamal M.

AU - Lu, Theresa T.

AU - Guttman-Yassky, Emma

AU - Lund, Amanda W.

AU - Anandasabapathy, Niroshana

AU - Naik, Shruti

PY - 2026/4/30

Y1 - 2026/4/30

N2 - Atopic diseases associated with allergens, as well as allergic diseases, frequently arise early in life; however, the age-dependent mechanisms governing immune responses to allergens remain poorly understood1. Here we find that in early life, exposure to common allergens triggers a distinct bifurcated immune response, simultaneously triggering type 17 inflammation in the skin and initiating canonical T helper 2 sensitization in the lymph nodes. This early-life γδ type 17-mediated dermatitis primes the exaggerated allergic lung inflammation upon secondary allergen exposure. Mechanistically, we find dendritic cell (DC)-mediated type 17 activation directly in the skin without requiring migration to lymph nodes; we term this state ‘peripheral immune inducer’ (pii) DC. CD301b+ conventional type 2 DCs acquire allergen, adopt the pii-DC state, produce IL-23 and activate local γδ type 17 cells independently of lymph-node engagement. The pii-DC state is enabled by the immature hypothalamic–pituitary–adrenal axis and physiologically low systemic glucocorticoids characteristic of early life2,3; DC-specific deletion of the glucocorticoid receptor recapitulates the pii-DC phenotype. These findings define a developmental checkpoint, set by neuroendocrine maturation, that enables in situ DC activation and immune induction, thereby shaping age-dependent responses to allergens.

AB - Atopic diseases associated with allergens, as well as allergic diseases, frequently arise early in life; however, the age-dependent mechanisms governing immune responses to allergens remain poorly understood1. Here we find that in early life, exposure to common allergens triggers a distinct bifurcated immune response, simultaneously triggering type 17 inflammation in the skin and initiating canonical T helper 2 sensitization in the lymph nodes. This early-life γδ type 17-mediated dermatitis primes the exaggerated allergic lung inflammation upon secondary allergen exposure. Mechanistically, we find dendritic cell (DC)-mediated type 17 activation directly in the skin without requiring migration to lymph nodes; we term this state ‘peripheral immune inducer’ (pii) DC. CD301b+ conventional type 2 DCs acquire allergen, adopt the pii-DC state, produce IL-23 and activate local γδ type 17 cells independently of lymph-node engagement. The pii-DC state is enabled by the immature hypothalamic–pituitary–adrenal axis and physiologically low systemic glucocorticoids characteristic of early life2,3; DC-specific deletion of the glucocorticoid receptor recapitulates the pii-DC phenotype. These findings define a developmental checkpoint, set by neuroendocrine maturation, that enables in situ DC activation and immune induction, thereby shaping age-dependent responses to allergens.

UR - https://www.scopus.com/pages/publications/105031236010

U2 - 10.1038/s41586-026-10162-x

DO - 10.1038/s41586-026-10162-x

M3 - Article

AN - SCOPUS:105031236010

SN - 0028-0836

VL - 652

SP - 1308

EP - 1317

JO - Nature

JF - Nature

IS - 8112

ER -

Peripheral immune-inducer dendritic cells drive early-life allergic inflammation

Abstract

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