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特应性皮炎生物治疗的发展现状:现状与未来展望。

The evolving landscape of biologic therapies for atopic dermatitis: Present and future perspective.

机构信息

Department of Dermatology, Icahn School of Medicine at Mount Sinai, New York, New York, USA.

Laboratory of Inflammatory Skin Diseases, Icahn School of Medicine at Mount Sinai, New York, New York, USA.

出版信息

Clin Exp Allergy. 2023 Feb;53(2):156-172. doi: 10.1111/cea.14263. Epub 2023 Jan 18.

Abstract

Atopic dermatitis (AD) is one of the most common, chronic inflammatory skin diseases with a significant physical, emotional and socioeconomic burden. In recent years the understanding of AD pathogenesis has expanded from the Th2-centred perspective, with the recognition of the involvement of other immune axes. In different AD endotypes, influenced by environment, genetics and race, transcriptomic profiles have identified differing contributions of multiple immune axes such as, Th17, Th22 and Th1. The enriched pathogenic model of AD has catalysed the development of numerous biologic therapies targeting a range of key molecules implicated in disease progression. Currently, dupilumab and tralokinumab, which both target the Th2 pathway, are the only approved biologic therapies for AD in the United States and Europe. New biologic therapies in development, however, target different Th2-pathway molecules along with cytokines in other immune axes, including Th17 and Th22, offering promise for varied treatments for this heterogeneous disease. As the biologic pipeline advances, the integration into clinical practice and approval of these experimental biologics may provide more effective, tailored therapeutic solutions and illuminate on the pathologic processes of AD across a broader, more diverse patient population.

摘要

特应性皮炎(AD)是最常见的慢性炎症性皮肤病之一,给患者的身体、心理和社会经济带来了巨大负担。近年来,人们对 AD 发病机制的认识已从以 Th2 为中心的观点扩展,认识到其他免疫轴的参与。在不同的 AD 表型中,受环境、遗传和种族的影响,转录组谱已确定多种免疫轴(如 Th17、Th22 和 Th1)的不同贡献。AD 丰富的发病模型促进了许多针对疾病进展中涉及的多种关键分子的生物疗法的发展。目前,dupilumab 和 tralokinumab 这两种靶向 Th2 通路的药物是美国和欧洲唯一批准用于 AD 的生物疗法。然而,正在开发的新型生物疗法针对不同的 Th2 通路分子以及其他免疫轴中的细胞因子,包括 Th17 和 Th22,为这种异质性疾病提供了多样化的治疗选择。随着生物制剂的研发进展,这些实验性生物制剂在临床实践中的整合和批准可能会提供更有效、更个体化的治疗方案,并阐明更广泛、更多样化的患者群体中 AD 的病理过程。

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