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Focus: Skin: Structural Basis for How Biologic Medicines Bind their Targets in Psoriasis Therapy

机译:重点:皮肤:生物医学在牛皮癣治疗中如何结合靶点的结构基础

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摘要

As biologic therapies become first line treatments for many inflammatory disorders, it becomes increasingly important for the practicing physician to be familiar with how these drugs function at the molecular level. This information is useful in making therapeutic decisions and helping patients understand their treatment options. It is critical to patient safety and clinical response that the molecular differences between these drugs inform prescribing practices. To this end, we present and analyze the available structural biology information about the biologics used in the treatment of psoriasis including inhibitors of tumor necrosis factor alpha (TNFα), interleukin-17 (IL-17), and interleukin-23 (IL-23). We describe and analyze the molecular surface character of known binding epitopes for medications in these classes, showing that significant differences exist in epitope location, hydrophobicity, and charge. Some of these differences can be correlated with clinical data, but our analysis ultimately points to the need for more structural information to allow for a better understanding of the structure-function relationship of biologic therapies.
机译:随着生物疗法成为许多炎症性疾病的一线治疗方法,对执业医师熟悉这些药物在分子水平上的作用变得越来越重要。此信息有助于做出治疗决策并帮助患者了解他们的治疗选择。这些患者之间的分子差异会影响处方操作,对患者安全和临床反应至关重要。为此,我们提出并分析了有关用于治疗牛皮癣的生物制剂的可用结构生物学信息,包括肿瘤坏死因子α(TNFα),白介素17(IL-17)和白介素23(IL-23)的抑制剂)。我们描述和分析这些类别的药物的已知结合表位的分子表面特征,表明在表位的位置,疏水性和电荷上存在显着差异。这些差异中的一些可以与临床数据相关联,但我们的分析最终指出需要更多的结构信息,以便更好地了解生物疗法的结构-功能关系。

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