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自身炎症:IL-1 在单基因自身炎症性疾病中的突出作用及其对常见疾病的影响。

Autoinflammation: the prominent role of IL-1 in monogenic autoinflammatory diseases and implications for common illnesses.

机构信息

National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

J Allergy Clin Immunol. 2009 Dec;124(6):1141-9; quiz 1150-1. doi: 10.1016/j.jaci.2009.11.016.

Abstract

The discovery of the genetic causes of a rare group of immune-mediated inflammatory conditions that mimic infections and allergic conditions in their clinical presentation and the molecular understanding of the function of the mutated molecules in these diseases has led to a revolution in our understanding of the pathogenesis of systemic and local inflammation. The proteins mutated in a number of these so-called autoinflammatory diseases are part of, or regulate the activity of, intracellular molecular complexes, the inflammasomes, that sense "danger" to the body and coordinate an initial immune response. Our understanding of specific triggers of the inflammasomes, coupled with the recognition that inflammasomes are critical for activation of the proinflammatory cytokine IL-1, has provided a rational and very effective target in the treatment of a number of these rare autoinflammatory diseases. In addition, the ongoing discovery of the role of inflammasomes and IL-1 activation and secretion in a number of genetically complex disorders have fundamentally changed our view of disease pathogenesis in a growing number of disorders that were heretofore not even thought of as "immunologic" diseases.

摘要

遗传原因的发现使得一组罕见的免疫介导的炎症性疾病的发病机制得到了阐明,这些疾病在临床表现上类似于感染和过敏反应。对这些疾病中突变分子功能的分子理解,导致了我们对全身性和局部炎症发病机制的理解发生了革命性的变化。在许多所谓的自身炎症性疾病中发生突变的蛋白质是细胞内分子复合物(炎症小体)的一部分,或者调节其活性,这些炎症小体能够感知对身体的“危险”,并协调初始免疫反应。我们对炎症小体特定触发因素的理解,加上对炎症小体对于促炎细胞因子 IL-1 的激活至关重要的认识,为治疗许多这类罕见的自身炎症性疾病提供了合理且非常有效的靶点。此外,炎症小体和 IL-1 激活和分泌在许多遗传复杂疾病中的作用的不断发现,从根本上改变了我们对越来越多的疾病发病机制的看法,这些疾病以前甚至不被认为是“免疫性”疾病。

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