High-sensitive sensory neurons exacerbate rosacea-like dermatitis in mice by activating γδ T cells directly

酒渣鼻 降钙素基因相关肽 伤害感受器 辣椒素 刺激 神经肽 脂毒素 免疫学 受体 医学 内分泌学 TRPV1型 伤害 皮肤病科 内科学 瞬时受体电位通道 痤疮
作者
Yiya Zhang,Tao Li,Han Zhao,X. Y. Xiao,Xi‐min Hu,Ben Wang,Yingxue Huang,Zhinan Yin,Yun Zhong,Yangfan Li,Ji Li
出处
期刊:Nature Communications [Nature Portfolio]
卷期号:15 (1) 被引量:4
标识
DOI:10.1038/s41467-024-50970-1
摘要

Rosacea patients show facial hypersensitivity to stimulus factors (such as heat and capsaicin); however, the underlying mechanism of this hyperresponsiveness remains poorly defined. Here, we show capsaicin stimulation in mice induces exacerbated rosacea-like dermatitis but has no apparent effect on normal skin. Nociceptor ablation substantially reduces the hyperresponsiveness of rosacea-like dermatitis. Subsequently, we find that γδ T cells express Ramp1, the receptor of the neuropeptide CGRP, and are in close contact with these nociceptors in the skin. γδ T cells are significantly increased in rosacea skin lesions and can be further recruited and activated by neuron-secreted CGRP. Rosacea-like dermatitis is reduced in T cell receptor δ-deficient (Tcrd−/−) mice, and the nociceptor-mediated aggravation of rosacea-like dermatitis is also reduced in these mice. In vitro experiments show that CGRP induces IL17A secretion from γδ T cells by regulating inflammation-related and metabolism-related pathways. Finally, rimegepant, a CGRP receptor antagonist, shows efficacy in the treatment of rosacea-like dermatitis. In conclusion, our findings demonstrate a neuron-CGRP-γδT cell axis that contributes to the hyperresponsiveness of rosacea, thereby showing that targeting CGRP is a potentially effective therapeutic strategy for rosacea. Rosacea is a common chronic inflammatory cutaneous disease that is exacerbated by heat and capsaicin pepper stimulation. Here the authors use a mouse model of rosacea and demonstrate functions of nociceptors, response to the neuropeptide CGRP and involvement of γδ T cells in the aggravation of rosacea like-disease.
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