Skin–gut crosstalk

IF 27.7 1区医学 Q1 IMMUNOLOGY

Nature Immunology Pub Date : 2025-04-30 DOI:10.1038/s41590-025-02158-y

Nicholas J. Bernard

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Abstract

Skin damage can have systemic effects but whether it can result in the priming of immune responses that are spatially removed from the skin is less clear. Data now published in Science Immunology show that cytokines released from damaged skin can function as endocrine adjuvants to prime normally tolerogenic gastrointestinal immune responses to the model food antigen ovalbumin, thereby driving humoral responses in mice. This ‘remote priming’ was demonstrated by oral gavage of ovalbumin in combination with tape stripping to damage the skin and resulted in ovalbumin-specific antibody responses. The same allergic sensitization was shown by two other means of acute skin damage (punch biopsy or intradermal acetone injection), a model of chronic atopic dermatitis (using calcipotriol) and in response to ultraviolet radiation damage. Although the cytokine signatures varied with the different skin damage methods, the researchers used cytokine immunizations and various cell-specific knockout mice to show that the cytokines IL-33 and TSLP were sufficient to drive similar ovalbumin-specific antibody responses to skin damage, in part by activation of group 2 innate lymphoid cells.

Original reference: Sci. Immunol. 10, eadn0688 (2025)

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皮肤损伤会产生全身性影响，但它是否会导致从皮肤上空间移除的免疫反应的启动尚不清楚。发表在《科学免疫学》（Science Immunology）杂志上的数据显示，受损皮肤释放的细胞因子可以作为内分泌佐剂，促进对模型食物抗原卵清蛋白的正常耐受性胃肠道免疫反应，从而驱动小鼠的体液反应。这种“远程启动”通过口服卵清蛋白与胶带剥离相结合来破坏皮肤并导致卵清蛋白特异性抗体反应来证明。急性皮肤损伤（穿刺活检或皮内注射丙酮）、慢性特应性皮炎模型（使用钙化三醇）和对紫外线辐射损伤的反应也显示出相同的过敏性致敏。尽管细胞因子特征随着不同的皮肤损伤方法而变化，但研究人员使用细胞因子免疫和各种细胞特异性敲除小鼠来证明细胞因子IL-33和TSLP足以驱动类似的卵清蛋白特异性抗体对皮肤损伤的反应，部分是通过激活2组先天淋巴样细胞。原始参考文献：Sci。免疫1 . 10,eadn0688 （2025）

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来源期刊

Nature Immunology 医学-免疫学

CiteScore

40.00

自引率

2.30%

发文量

248

审稿时长

4-8 weeks

期刊介绍： Nature Immunology is a monthly journal that publishes the highest quality research in all areas of immunology. The editorial decisions are made by a team of full-time professional editors. The journal prioritizes work that provides translational and/or fundamental insight into the workings of the immune system. It covers a wide range of topics including innate immunity and inflammation, development, immune receptors, signaling and apoptosis, antigen presentation, gene regulation and recombination, cellular and systemic immunity, vaccines, immune tolerance, autoimmunity, tumor immunology, and microbial immunopathology. In addition to publishing significant original research, Nature Immunology also includes comments, News and Views, research highlights, matters arising from readers, and reviews of the literature. The journal serves as a major conduit of top-quality information for the immunology community.