MRC Laboratory of Molecular Biology, Francis Crick Avenue, Cambridge CB2 0QH, UK.
Division of Structural Biology, The Institute of Cancer Research, London SW3 3RP, UK.
Nat Commun. 2015 Jul 2;6:7573. doi: 10.1038/ncomms8573.
The proteasome is a highly regulated protease complex fundamental for cell homeostasis and controlled cell cycle progression. It functions by removing a wide range of specifically tagged proteins, including key cellular regulators. Here we present the structure of the human 20S proteasome core bound to a substrate analogue inhibitor molecule, determined by electron cryo-microscopy (cryo-EM) and single-particle analysis at a resolution of around 3.5 Å. Our map allows the building of protein coordinates as well as defining the location and conformation of the inhibitor at the different active sites. These results open new prospects to tackle the proteasome functional mechanisms. Moreover, they also further demonstrate that cryo-EM is emerging as a realistic approach for general structural studies of protein-ligand interactions.
蛋白酶体是一种高度调控的蛋白酶复合物,对细胞内稳态和细胞周期进程的控制至关重要。它通过去除广泛的、具有特定标记的蛋白质来发挥作用,包括关键的细胞调节剂。在这里,我们通过电子晶体学(cryo-EM)和单颗粒分析,以约 3.5 Å 的分辨率,展示了与底物类似物抑制剂分子结合的人源 20S 蛋白酶体核心的结构。我们的图谱允许构建蛋白质坐标,并确定抑制剂在不同活性部位的位置和构象。这些结果为研究蛋白酶体的功能机制开辟了新的前景。此外,它们还进一步证明,cryo-EM 正在成为研究蛋白质-配体相互作用的一般结构的一种可行方法。
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