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组胺H1和H4受体在特应性皮炎中的作用:从基础研究到临床研究

The role of histamine H1 and H4 receptors in atopic dermatitis: from basic research to clinical study.

作者信息

Ohsawa Yusuke, Hirasawa Noriyasu

机构信息

Laboratory of Pharmacotherapy of Life-Style Related Diseases, Graduate School of Pharmaceutical Sciences, Tohoku University, Miyagi, Japan.

出版信息

Allergol Int. 2014 Dec;63(4):533-42. doi: 10.2332/allergolint.13-RA-0675.

DOI:10.2332/allergolint.13-RA-0675
PMID:25249063
Abstract

Histamine plays important roles in inflammation and nervous irritability in allergic disorders, including atopic dermatitis (AD). It has been shown to regulate the expression of pruritic factors, such as nerve growth factor and semaphorin 3A, in skin keratinocytes via histamine H1 receptor (H1R). Furthermore, H1R antagonist reduced the level of IL-31, a cytokine involving the skin barrier and pruritus, in chronic dermatitis lesions in NC/Nga mice and patients with AD. Histamine plays roles in the induction of allergic inflammation by activating eosinophils, mast cells, basophils, and Th2 cells via histamine H4 receptor (H4R). H4R, in addition to H1R, is expressed on sensory neurons, and a decrease in scratching behaviors was observed in H4R-deficient mice and mice treated with a H4R antagonist. We found that the combined administration of H1R and H4R antagonists inhibited the itch response and chronic allergic inflammation, and had a pharmacological effect similar to that of prednisolone. Although the oral administration of H1R antagonists is widely used to treat AD, it is not very effective. In contrast, JNJ39758979, a novel H4R antagonist, had marked effects against pruritus in Japanese patients with AD in a phase II clinical trial. Next generation antihistaminic agents possessing H1R and H4R antagonistic actions may be a potent therapeutic drug for AD.

摘要

组胺在包括特应性皮炎(AD)在内的过敏性疾病的炎症和神经兴奋性中发挥重要作用。研究表明,它可通过组胺H1受体(H1R)调节皮肤角质形成细胞中瘙痒因子的表达,如神经生长因子和信号素3A。此外,H1R拮抗剂可降低NC/Nga小鼠和AD患者慢性皮炎皮损中白细胞介素-31(一种涉及皮肤屏障和瘙痒的细胞因子)的水平。组胺通过组胺H4受体(H4R)激活嗜酸性粒细胞、肥大细胞、嗜碱性粒细胞和Th2细胞,从而在过敏性炎症的诱导中发挥作用。除H1R外,H4R也表达于感觉神经元上,在H4R缺陷小鼠和用H4R拮抗剂处理的小鼠中观察到抓挠行为减少。我们发现,联合给予H1R和H4R拮抗剂可抑制瘙痒反应和慢性过敏性炎症,且具有与泼尼松龙相似的药理作用。虽然口服H1R拮抗剂广泛用于治疗AD,但效果并不理想。相比之下,新型H4R拮抗剂JNJ39758979在一项II期临床试验中对日本AD患者的瘙痒有显著疗效。具有H1R和H4R拮抗作用的新一代抗组胺药可能是治疗AD的有效药物。

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