de Jesús-Gil Carmen, Sans-de SanNicolàs Lídia, García-Jiménez Irene, Ferran Marta, Celada Antonio, Chiriac Anca, Pujol Ramon M, Santamaria-Babí Luis F
Translational Immunology, Department of Cellular Biology, Physiology, and Immunology, Faculty of Biology, Universitat de Barcelona, Parc Científic de Barcelona, Barcelona, Spain.
Department of Dermatology, Hospital del Mar, Institut Hospital del Mar d'Investigacions Mèdiques (IMIM), Universitat Autònoma de Barcelona, Barcelona, Spain.
Front Immunol. 2021 Mar 23;12:652613. doi: 10.3389/fimmu.2021.652613. eCollection 2021.
Circulating memory T cells are heterogeneous in their tissue tropism. The skin-seeking T cell subset expresses the cutaneous lymphocyte-associated antigen (CLA) on their surface. CLA memory T cells not only migrate from blood to skin but also recirculate between blood and skin. Studying CLA memory T cells in cutaneous diseases has allowed a better understanding of immune-inflammatory mechanisms that take place. The analysis of the phenotypical features of these cells, their antigen specificity, cytokine production profile, and changes in relationship to clinical status and therapies among other characteristics have led to the concept that they constitute peripheral cellular biomarkers in T cell-mediated cutaneous conditions. CLA memory T cells are of relevance in the pathogenesis of several cutaneous diseases, such as psoriasis (PSO), atopic dermatitis, vitiligo, and drug-induced allergic reactions, to name a few. The interaction of circulating CLA T cells with skin-resident cells has been investigated in different coculture models made out of clinical samples. Interestingly, microbes that are present in the skin or related with human skin diseases are preferentially recognized by CLA T cells. Thus, the interaction of with CLA T cells in PSO is providing novel concepts that help to understand disease immunopathogenesis. The goal of this review is to present latest results in the field of CLA T cells in T cell-mediated inflammatory skin diseases and their translational relevance for human immunodermatology.
循环记忆T细胞在组织嗜性方面具有异质性。趋皮肤T细胞亚群在其表面表达皮肤淋巴细胞相关抗原(CLA)。CLA记忆T细胞不仅从血液迁移至皮肤,还在血液和皮肤之间再循环。对皮肤疾病中CLA记忆T细胞的研究有助于更好地理解其中发生的免疫炎症机制。对这些细胞的表型特征、抗原特异性、细胞因子产生谱以及与临床状态和治疗相关的变化等其他特征的分析,引出了它们在T细胞介导的皮肤疾病中构成外周细胞生物标志物的概念。CLA记忆T细胞与多种皮肤疾病的发病机制相关,如银屑病(PSO)、特应性皮炎、白癜风和药物性过敏反应等。在由临床样本构建的不同共培养模型中,已对循环CLA T细胞与皮肤驻留细胞的相互作用进行了研究。有趣的是,皮肤中存在的或与人类皮肤疾病相关的微生物优先被CLA T细胞识别。因此,PSO中 与CLA T细胞的相互作用提供了有助于理解疾病免疫发病机制的新观念。本综述的目的是介绍T细胞介导的炎症性皮肤病领域中CLA T细胞的最新研究结果及其对人类免疫皮肤病学的转化意义。
