无定形药物阿图利黄酮的原子级结构 核磁共振晶体学
Atomic-level structure of the amorphous drug atuliflapon NMR crystallography.
作者信息
Holmes Jacob B, Torodii Daria, Balodis Martins, Cordova Manuel, Hofstetter Albert, Paruzzo Federico, Nilsson Lill Sten O, Eriksson Emma, Berruyer Pierrick, Simões de Almeida Bruno, Quayle Mike, Norberg Stefan, Ankarberg Anna Svensk, Schantz Staffan, Emsley Lyndon
机构信息
Institut des Sciences et Ingénierie Chimiques, Ecole Polytechnique Fédérale de Lausanne (EPFL), CH-1015 Lausanne, Switzerland.
National Centre for Computational Design and Discovery of Novel Materials MARVEL, Ecole Polytechnique Fédérale de Lausanne (EPFL), CH-1015 Lausanne, Switzerland.
出版信息
Faraday Discuss. 2025 Jan 8;255(0):342-354. doi: 10.1039/d4fd00078a.
We determine the complete atomic-level structure of the amorphous form of the drug atuliflapon, a 5-lipooxygenase activating protein (FLAP) inhibitor, chemical-shift-driven NMR crystallography. The ensemble of preferred structures allows us to identify a number of specific conformations and interactions that stabilize the amorphous structure. These include preferred hydrogen-bonding motifs with water and with other drug molecules, as well as conformations of the cyclohexane and pyrazole rings that stabilize structure by indirectly allowing for optimization of hydrogen bonding.
我们通过化学位移驱动的核磁共振晶体学确定了药物阿图利黄酮(一种5-脂氧合酶激活蛋白(FLAP)抑制剂)无定形形式的完整原子水平结构。优选结构的集合使我们能够识别出许多稳定无定形结构的特定构象和相互作用。这些包括与水和其他药物分子的优选氢键基序,以及通过间接允许氢键优化来稳定结构的环己烷和吡唑环的构象。
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