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首页> 外文期刊>Current Rheumatology Reviews >Systemic Sclerosis: From Pathogenesis Towards Targeted Immunotherapies
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Systemic Sclerosis: From Pathogenesis Towards Targeted Immunotherapies

机译:系统性硬化症:从发病机制到针对性的免疫治疗

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摘要

Systemic sclerosis (SSc), a chronic disease with widespread collagen deposition, has three pathogenetic facets: immune activation, microvasculopathy and fibroblast activation. Immune activation and microvasculopathy occur very early in the disease process, and inflammatory infiltrates in the skin are restricted in early-phase disease. There is good evidence that fibroblast activation with collagen production may be triggered by the immune system. In early-phase disease, we slowly move from general immunosuppression to therapeutically targeting specific molecules involved in immune activation, such as T cell-directed targets, B cell-directed targets, cytokine targets, and tyrosine kinases targets.
机译:系统性硬化症(SSc)是一种具有大量胶原蛋白沉积的慢性疾病,具有三个致病性方面:免疫激活,微血管病变和成纤维细胞激活。免疫激活和微血管病变发生在疾病过程的早期,而皮肤的炎性浸润在早期疾病中受到限制。有充分的证据表明,免疫系统可触发成纤维细胞活化并产生胶原蛋白。在早期疾病中,我们逐渐从一般的免疫抑制转向治疗性靶向与免疫激活有关的特定分子,例如T细胞定向靶,B细胞定向靶,细胞因子靶和酪氨酸激酶靶。

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