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硬皮病病理生理学最新进展:特别关注免疫炎症事件

Update on pathophysiology of scleroderma with special reference to immunoinflammatory events.

作者信息

Chizzolini Carlo

机构信息

Immunology and Allergy, University Hospital, School of Medicine, Geneva, Switzerland.

出版信息

Ann Med. 2007;39(1):42-53. doi: 10.1080/07853890601098152.

Abstract

Scleroderma or systemic sclerosis (SSc) is a complex disease in which the vasculopathy and the activation of the immune system with production of inflammatory mediators lead to dysregulated fibroblast activation. The resulting excessive deposition of collagens and other extracellular matrix proteins ends in fibrosis and organ dysfunction. The cause is unknown, but environmental factors are thought to play a role by triggering abnormal responses in genetically susceptible hosts. The recent past has witnessed important advances in the definition of mechanisms that underlie the persistent activation in fibroblasts of genes involved in uncontrolled fibrosis, a hallmark of SSc. These include the preferential production of type 2 T cell cytokines in target organs, the presence of autoantibodies with fibroblast-activating capacities, the production of vasoconstrictive mediators that impact on fibroblast biosynthetic properties, the transforming growth factor-beta-related metabolic signature, and the presence of altered signaling pathways in fibroblasts. Furthermore, while no animal models recapitulate all the features of SSc, they have been instrumental for assessing the relevance of specific processes to the development of fibrosis. More importantly, some of the research findings are leading to therapies that target altered processes with the potential of changing the prognosis of some dismal aspects of the disease.

摘要

硬皮病或系统性硬化症(SSc)是一种复杂的疾病,其中血管病变以及免疫系统激活并产生炎症介质会导致成纤维细胞活化失调。由此产生的胶原蛋白和其他细胞外基质蛋白过度沉积最终会导致纤维化和器官功能障碍。病因尚不清楚,但环境因素被认为通过在基因易感宿主中引发异常反应而发挥作用。最近,在确定参与不受控制的纤维化(SSc的一个标志)的基因在成纤维细胞中持续激活的机制方面取得了重要进展。这些机制包括靶器官中2型T细胞细胞因子的优先产生、具有成纤维细胞激活能力的自身抗体的存在、影响成纤维细胞生物合成特性的血管收缩介质的产生、转化生长因子-β相关的代谢特征以及成纤维细胞中信号通路的改变。此外,虽然没有动物模型能概括SSc的所有特征,但它们对于评估特定过程与纤维化发展的相关性很有帮助。更重要的是,一些研究结果正在促成针对改变的过程的疗法,这些疗法有可能改变该疾病某些严峻方面的预后。

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