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Immunopathogenesis of Pediatric Localized Scleroderma

机译:小儿局限性硬皮病的免疫发病机制

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摘要

Localized scleroderma (LS) is a complex disease characterized by a mixture of inflammation and fibrosis of the skin that, especially in the pediatric population, also affects extracutaneous tissues ranging from muscle to the central nervous system. Although developmental origins have been hypothesized, evidence points to LS as a systemic autoimmune disorder, as there is a strong correlation to family history of autoimmune disease, the presence of shared HLA types with rheumatoid arthritis, high frequency of auto-antibodies, and elevated circulating chemokines and cytokines associated with T-helper cell, IFNγ, and other inflammatory pathways. This inflammatory phenotype of the peripheral blood is reflected in the skin via microarray, RNA Sequencing and tissue staining. Research is underway to identify the key players in the pathogenesis of LS, but close approximation of inflammatory lymphocytic and macrophage infiltrate with collagen and fibroblasts deposition supports the notion that LS is a disease of inflammatory driven fibrosis. The immune system is dynamic and undergoes changes during childhood, and we speculate on how the unique features of the immune system in childhood could potentially contribute to some of the differences in LS between children and adults. Interestingly, the immune phenotype in pediatric LS resembles to some extent the healthy adult cellular phenotype, possibly supporting accelerated maturation of the immune system in LS. We discuss future directions in better understanding the pathophysiology of and how to better treat pediatric LS.
机译:局部硬皮病(LS)是一种复杂的疾病,其特征在于皮肤的炎症和纤维化混合在一起,尤其是在儿科人群中,还影响从肌肉到中枢神经系统的皮外组织。尽管已经假设了发育起源,但证据表明LS是系统性自身免疫疾病,因为与自身免疫疾病的家族史,类风湿性关节炎共有HLA类型,自身抗体的高频率以及循环血循环密切相关与T辅助细胞,IFNγ和其他炎症途径相关的趋化因子和细胞因子。外周血的这种炎症表型通过微阵列,RNA测序和组织染色反映在皮肤上。正在进行研究以鉴定LS的发病机理中的关键因素,但是与胶原和成纤维细胞沉积密切相关的炎性淋巴细胞和巨噬细胞浸润,支持了LS是炎性驱动性纤维化疾病的观点。免疫系统是动态的,在童年时期会发生变化,我们推测童年时期免疫系统的独特特征如何可能导致儿童和成人之间的LS差异。有趣的是,小儿LS中的免疫表型在某种程度上类似于健康的成人细胞表型,可能支持LS中免疫系统的加速成熟。我们讨论了未来的方向,以更好地了解小儿LS的病理生理以及如何更好地治疗小儿LS。

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