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Innovative antifibrotic therapies in systemic sclerosis

机译:全身性硬化症的创新抗纤维化疗法

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摘要

Purpose of Review: Fibrosis is a key feature of systemic sclerosis (SSc) and arises from excessive release of collagens by pathologically activated fibroblasts. Affecting the skin and many internal organs, fibrosis represents a major cause for the high morbidity and mortality in SSc. So far, effective therapies to treat fibrosis in SSc and other fibrotic diseases are not available in clinical routine. Nevertheless, promising antifibrotic agents are emerging from translational studies with some having already entered clinical trials. Recent Findings: In this review, we focus on recent advances in the development of antifibrotic treatment strategies in SSc. We have selected for targeted therapeutic approaches that have proven high efficacy and tolerability in preclinical fibrosis models of SSc and/or are already in clinical evaluation. Applying these criteria, we discuss a large repertory of candidate antifibrotic therapies that block inflammatory pathways, inhibit profibrotic growth factors, modulate epigenetic signaling, and interfere with morphogenic pathways. Summary: Many antifibrotic candidate therapies have proven efficacy and tolerability in preclinical models of SSc. So far, early clinical studies have tested only few of these agents. Besides discovering novel molecular treatment strategies, SSc research will now have to translate its findings into clinical practice.
机译:审查目的:纤维化是系统性硬化症(SSc)的一个关键特征,它是由病理激活的成纤维细胞过度释放胶原蛋白引起的。纤维化影响皮肤和许多内部器官,是SSc高发病率和高死亡率的主要原因。到目前为止,在临床常规治疗中尚无有效的疗法可治疗SSc和其他纤维化疾病中的纤维化。然而,转化研究正在出现有希望的抗纤维化药物,其中一些已经进入临床试验。最新发现:在这篇综述中,我们着重于SSc抗纤维化治疗策略发展的最新进展。我们选择了针对性治疗方法,这些方法在SSc的临床前纤维化模型中已证明具有很高的疗效和耐受性,并且/或者已经在临床评估中。应用这些标准,我们讨论了候选抗纤维化疗法的全部文献,这些疗法可阻断炎症途径,抑制纤维化生长因子,调节表观遗传信号,并干扰形态发生途径。摘要:许多抗纤维化候选疗法在SSc的临床前模型中均已证明具有疗效和耐受性。迄今为止,早期的临床研究仅测试了其中的几种药物。除了发现新颖的分子治疗策略外,SSc研究现在还必须将其发现转化为临床实践。

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