首页> 美国卫生研究院文献>Protein Science : A Publication of the Protein Society >High-resolution structure of the stable plasminogen activator inhibitor type-1 variant 14-1B in its proteinase-cleaved form: A new tool for detailed interaction studies and modeling
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High-resolution structure of the stable plasminogen activator inhibitor type-1 variant 14-1B in its proteinase-cleaved form: A new tool for detailed interaction studies and modeling

机译:稳定的纤溶酶原激活物抑制剂1型变异体14-1B(以蛋白酶切割的形式)的高分辨率结构:进行详细相互作用研究和建模的新工具

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摘要

Wild-type plasminogen activator inhibitor type-1 (PAI-1) rapidly converts to the inactive latent state under conditions of physiological pH and temperature. For in vivo studies of active PAI-1 in cell culture and in vivo model systems, the 14-1B PAI-1 mutant (N150H-K154T-Q319L-M354I), with its stabilized active conformation, has thus become the PAI-1 of choice. As a consequence of the increased stability, the only two forms likely to be encountered are the active or the cleaved form, the latter either free or complexed with target proteinase. We hereby report the first structure of the stable 14-1B PAI-1 variant in its reactive center cleaved form, to a resolution of 2.0 Å. The >99% complete structure represents the highest resolved structure of free cleaved PAI-1. This high-resolution structure should be of great use for drug target development and for modeling protein–protein interactions such as those of PAI-1 with vitronectin.
机译:在生理pH和温度条件下,野生型纤溶酶原激活物抑制剂1型(PAI-1)迅速转变为非活性潜伏状态。为了在细胞培养和体内模型系统中进行活性PAI-1的体内研究,具有稳定的活性构象的14-1B PAI-1突变体(N150H-K154T-Q319L-M354I)已成为PAI-1的选择。由于增加的稳定性,可能遇到的仅有的两种形式是活性形式或裂解形式,后者游离或与靶蛋白酶复合。我们在此报告稳定的14-1B PAI-1变体以其反应性中心裂解形式的第一个结构,其分辨率为2.0。 > 99%的完整结构代表了游离切割的PAI-1的最高解析结构。这种高分辨率结构对于药物靶标开发和建立蛋白质-蛋白质相互作用(例如PAI-1与玻连蛋白的相互作用)应该具有很大的用途。

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