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人白三烯C4合酶合成炎症介质的结构基础。

Structural basis for synthesis of inflammatory mediators by human leukotriene C4 synthase.

作者信息

Martinez Molina Daniel, Wetterholm Anders, Kohl Andreas, McCarthy Andrew A, Niegowski Damian, Ohlson Eva, Hammarberg Tove, Eshaghi Said, Haeggström Jesper Z, Nordlund Pär

机构信息

Division of Biophysics, Karolinska Institutet, 17177 Stockholm, Sweden.

出版信息

Nature. 2007 Aug 2;448(7153):613-6. doi: 10.1038/nature06009. Epub 2007 Jul 15.

DOI:10.1038/nature06009
PMID:17632546
Abstract

Cysteinyl leukotrienes are key mediators in inflammation and have an important role in acute and chronic inflammatory diseases of the cardiovascular and respiratory systems, in particular bronchial asthma. In the biosynthesis of cysteinyl leukotrienes, conversion of arachidonic acid forms the unstable epoxide leukotriene A4 (LTA4). This intermediate is conjugated with glutathione (GSH) to produce leukotriene C4 (LTC4) in a reaction catalysed by LTC4 synthase: this reaction is the key step in cysteinyl leukotriene formation. Here we present the crystal structure of the human LTC4 synthase in its apo and GSH-complexed forms to 2.00 and 2.15 A resolution, respectively. The structure reveals a homotrimer, where each monomer is composed of four transmembrane segments. The structure of the enzyme in complex with substrate reveals that the active site enforces a horseshoe-shaped conformation on GSH, and effectively positions the thiol group for activation by a nearby arginine at the membrane-enzyme interface. In addition, the structure provides a model for how the omega-end of the lipophilic co-substrate is pinned at one end of a hydrophobic cleft, providing a molecular 'ruler' to align the reactive epoxide at the thiol of glutathione. This provides new structural insights into the mechanism of LTC4 formation, and also suggests that the observed binding and activation of GSH might be common for a family of homologous proteins important for inflammatory and detoxification responses.

摘要

半胱氨酰白三烯是炎症中的关键介质,在心血管和呼吸系统的急慢性炎症性疾病,尤其是支气管哮喘中发挥重要作用。在半胱氨酰白三烯的生物合成过程中,花生四烯酸的转化形成不稳定的环氧化白三烯A4(LTA4)。该中间体与谷胱甘肽(GSH)结合,在LTC4合酶催化的反应中生成白三烯C4(LTC4):此反应是半胱氨酰白三烯形成的关键步骤。在此,我们分别给出了人LTC4合酶无配体形式和与GSH结合形式的晶体结构,分辨率分别为2.00 Å和2.15 Å。该结构显示为同三聚体,其中每个单体由四个跨膜片段组成。与底物结合的酶结构表明,活性位点使GSH呈马蹄形构象,并有效地将硫醇基团定位在膜 - 酶界面附近的精氨酸处进行激活。此外,该结构提供了一个模型,说明亲脂性共底物的ω端如何固定在疏水裂缝的一端,提供一个分子“尺子”来使反应性环氧化物与谷胱甘肽的硫醇对齐。这为LTC4形成机制提供了新的结构见解,也表明所观察到的GSH的结合和激活可能对于对炎症和解毒反应重要的同源蛋白家族是常见的。

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