Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice

Chen Huang; Pei Yi Sun; Yiming Jiang; Yuandong Liu; Zhichao Liu; Shao Ling Han; Bao Shan Wang; Yong Xin Huang; An Ran Ren; Jian Fei Lu; Qin Jiang; Ying Li; Michael X. Zhu; Zhirong Yao; Yang Tian; Xin Qi; Wei Guang Li; Tian Le Xu

doi:10.1038/s41467-024-49577-3

Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice

Chen Huang
, Pei Yi Sun
, Yiming Jiang
, Yuandong Liu
, Zhichao Liu
, Shao Ling Han
, Bao Shan Wang
, Yong Xin Huang
, An Ran Ren
, Jian Fei Lu
, Qin Jiang
, Ying Li
, Michael X. Zhu
, Zhirong Yao
, Yang Tian
, Xin Qi^*
, Wei Guang Li^*
, Tian Le Xu^*

^*此作品的通讯作者

化学与分子工程学院

Shanghai Jiao Tong University
East China Normal University
University of Texas Health Science Center at Houston
Fudan University
Shanghai Research Center for Brain Science and Brain-Inspired Intelligence

科研成果: 期刊稿件 › 文章 › 同行评审

23 引用（Scopus）

摘要

Psoriasis is an immune-mediated skin disease associated with neurogenic inflammation, but the underlying molecular mechanism remains unclear. We demonstrate here that acid-sensing ion channel 3 (ASIC3) exacerbates psoriatic inflammation through a sensory neurogenic pathway. Global or nociceptor-specific Asic3 knockout (KO) in female mice alleviates imiquimod-induced psoriatic acanthosis and type 17 inflammation to the same extent as nociceptor ablation. However, ASIC3 is dispensable for IL-23-induced psoriatic inflammation that bypasses the need for nociceptors. Mechanistically, ASIC3 activation induces the activity-dependent release of calcitonin gene-related peptide (CGRP) from sensory neurons to promote neurogenic inflammation. Botulinum neurotoxin A and CGRP antagonists prevent sensory neuron-mediated exacerbation of psoriatic inflammation to similar extents as Asic3 KO. In contrast, replenishing CGRP in the skin of Asic3 KO mice restores the inflammatory response. These findings establish sensory ASIC3 as a critical constituent in psoriatic inflammation, and a promising target for neurogenic inflammation management.

源语言	英语
文章编号	5288
期刊	Nature Communications
卷	15
期	1
DOI	https://doi.org/10.1038/s41467-024-49577-3
出版状态	已出版 - 12月 2024

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Huang, C., Sun, P. Y., Jiang, Y., Liu, Y., Liu, Z., Han, S. L., Wang, B. S., Huang, Y. X., Ren, A. R., Lu, J. F., Jiang, Q., Li, Y., Zhu, M. X., Yao, Z., Tian, Y., Qi, X., Li, W. G., & Xu, T. L. (2024). Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice. Nature Communications, 15(1), 文章 5288. https://doi.org/10.1038/s41467-024-49577-3

@article{813b40190edd44f498b39dbdde397532,

title = "Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice",

abstract = "Psoriasis is an immune-mediated skin disease associated with neurogenic inflammation, but the underlying molecular mechanism remains unclear. We demonstrate here that acid-sensing ion channel 3 (ASIC3) exacerbates psoriatic inflammation through a sensory neurogenic pathway. Global or nociceptor-specific Asic3 knockout (KO) in female mice alleviates imiquimod-induced psoriatic acanthosis and type 17 inflammation to the same extent as nociceptor ablation. However, ASIC3 is dispensable for IL-23-induced psoriatic inflammation that bypasses the need for nociceptors. Mechanistically, ASIC3 activation induces the activity-dependent release of calcitonin gene-related peptide (CGRP) from sensory neurons to promote neurogenic inflammation. Botulinum neurotoxin A and CGRP antagonists prevent sensory neuron-mediated exacerbation of psoriatic inflammation to similar extents as Asic3 KO. In contrast, replenishing CGRP in the skin of Asic3 KO mice restores the inflammatory response. These findings establish sensory ASIC3 as a critical constituent in psoriatic inflammation, and a promising target for neurogenic inflammation management.",

author = "Chen Huang and Sun, \{Pei Yi\} and Yiming Jiang and Yuandong Liu and Zhichao Liu and Han, \{Shao Ling\} and Wang, \{Bao Shan\} and Huang, \{Yong Xin\} and Ren, \{An Ran\} and Lu, \{Jian Fei\} and Qin Jiang and Ying Li and Zhu, \{Michael X.\} and Zhirong Yao and Yang Tian and Xin Qi and Li, \{Wei Guang\} and Xu, \{Tian Le\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

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doi = "10.1038/s41467-024-49577-3",

language = "英语",

volume = "15",

journal = "Nature Communications",

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T1 - Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice

AU - Huang, Chen

AU - Sun, Pei Yi

AU - Jiang, Yiming

AU - Liu, Yuandong

AU - Liu, Zhichao

AU - Han, Shao Ling

AU - Wang, Bao Shan

AU - Huang, Yong Xin

AU - Ren, An Ran

AU - Lu, Jian Fei

AU - Jiang, Qin

AU - Li, Ying

AU - Zhu, Michael X.

AU - Yao, Zhirong

AU - Tian, Yang

AU - Qi, Xin

AU - Li, Wei Guang

AU - Xu, Tian Le

PY - 2024/12

Y1 - 2024/12

N2 - Psoriasis is an immune-mediated skin disease associated with neurogenic inflammation, but the underlying molecular mechanism remains unclear. We demonstrate here that acid-sensing ion channel 3 (ASIC3) exacerbates psoriatic inflammation through a sensory neurogenic pathway. Global or nociceptor-specific Asic3 knockout (KO) in female mice alleviates imiquimod-induced psoriatic acanthosis and type 17 inflammation to the same extent as nociceptor ablation. However, ASIC3 is dispensable for IL-23-induced psoriatic inflammation that bypasses the need for nociceptors. Mechanistically, ASIC3 activation induces the activity-dependent release of calcitonin gene-related peptide (CGRP) from sensory neurons to promote neurogenic inflammation. Botulinum neurotoxin A and CGRP antagonists prevent sensory neuron-mediated exacerbation of psoriatic inflammation to similar extents as Asic3 KO. In contrast, replenishing CGRP in the skin of Asic3 KO mice restores the inflammatory response. These findings establish sensory ASIC3 as a critical constituent in psoriatic inflammation, and a promising target for neurogenic inflammation management.

AB - Psoriasis is an immune-mediated skin disease associated with neurogenic inflammation, but the underlying molecular mechanism remains unclear. We demonstrate here that acid-sensing ion channel 3 (ASIC3) exacerbates psoriatic inflammation through a sensory neurogenic pathway. Global or nociceptor-specific Asic3 knockout (KO) in female mice alleviates imiquimod-induced psoriatic acanthosis and type 17 inflammation to the same extent as nociceptor ablation. However, ASIC3 is dispensable for IL-23-induced psoriatic inflammation that bypasses the need for nociceptors. Mechanistically, ASIC3 activation induces the activity-dependent release of calcitonin gene-related peptide (CGRP) from sensory neurons to promote neurogenic inflammation. Botulinum neurotoxin A and CGRP antagonists prevent sensory neuron-mediated exacerbation of psoriatic inflammation to similar extents as Asic3 KO. In contrast, replenishing CGRP in the skin of Asic3 KO mice restores the inflammatory response. These findings establish sensory ASIC3 as a critical constituent in psoriatic inflammation, and a promising target for neurogenic inflammation management.

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U2 - 10.1038/s41467-024-49577-3

DO - 10.1038/s41467-024-49577-3

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AN - SCOPUS:85196517907

SN - 2041-1723

VL - 15

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 5288

ER -

Sensory ASIC3 channel exacerbates psoriatic inflammation via a neurogenic pathway in female mice

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