Inhibition of IL-1, IL-6, and TNF-alpha in immune-mediated inflammatory diseases.

Springer seminars in immunopathology Pub Date : 2006-06-01 Epub Date: 2006-05-09 DOI:10.1007/s00281-006-0012-9
Burkhard Möller, Peter M Villiger
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引用次数: 129

Abstract

Blockade of cytokines, particularly of tumour necrosis factor alpha (TNF-alpha), in immuno-inflammatory diseases, has led to the greatest advances in medicine of recent years. We did a thorough review of the literature with a focus on inflammation models in rodents on modified gene expression or bioactivity for IL-1, IL-6, and TNF-alpha, and we summarized the results of randomized controlled clinical trials in human disease. What we have learned herewith is that important information can be achieved by the use of animal models in complex, immune-mediated diseases. However, a clear ranking for putative therapeutic targets appears difficult to obtain from an experimental approach alone. This is primarily due to the fact that none of the disease models has proven to cover more than one crucial pathogenetic aspect of the complex cascade of events leading to characteristic clinical disease signs and symptoms. This supports the notion that the addressed human immune-mediated diseases are polygenic and the summation of genetic, perhaps epigenetic, and environmental factors. Nevertheless, it has become apparent, so far, that TNF-alpha is of crucial importance in the development of antigen-dependent and antigen-independent models of inflammation, and that these results correlate well with clinical success. With some delay, clinical trials in conditions having some relationship with rheumatoid arthritis (RA) indicate new opportunities for blocking IL-1 or IL-6 therapeutically. It appears, therefore, that a translational approach with critical, mutual reflection of simultaneously performed experiments and clinical trials is important for rapid identification of new targets and development of novel treatment options in complex, immune-mediated, inflammatory diseases.

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IL-1、IL-6和tnf - α在免疫介导炎性疾病中的抑制作用
在免疫炎性疾病中,细胞因子的阻断,特别是肿瘤坏死因子α (tnf - α)的阻断,导致了近年来医学的最大进步。我们对有关IL-1、IL-6和tnf - α基因表达或生物活性改变的啮齿动物炎症模型的文献进行了全面的回顾,并总结了人类疾病随机对照临床试验的结果。我们在此了解到的是,在复杂的免疫介导疾病中使用动物模型可以获得重要信息。然而,对假定的治疗靶点的明确排序似乎很难单独从实验方法中获得。这主要是由于没有一种疾病模型被证明涵盖了导致特征性临床疾病体征和症状的复杂级联事件的一个以上关键的发病方面。这支持了这样一种观点,即所讨论的人类免疫介导的疾病是多基因的,是遗传因素,也许是表观遗传因素和环境因素的总和。然而,到目前为止,已经很明显,tnf - α在抗原依赖性和抗原非依赖性炎症模型的发展中起着至关重要的作用,并且这些结果与临床成功密切相关。虽然有些延迟,但与类风湿关节炎(RA)有一定关系的临床试验表明,阻断IL-1或IL-6的治疗有了新的机会。因此,对同时进行的实验和临床试验进行关键的相互反映的转化方法对于快速确定复杂的免疫介导的炎症性疾病的新靶点和开发新的治疗方案至关重要。
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