胞质分裂
激酶
蛋白激酶结构域
生物物理学
细胞生物学
化学
可药性
小分子
生物
生物化学
细胞
细胞分裂
基因
突变体
作者
Sebastian Mathea,E. Salah,C. Tallant,Deep Chatterjee,Benedict‐Tilman Berger,Rebecca Konietzny,Susanne Müller,Benedikt M. Kessler,Stefan Knapp
摘要
The human protein kinase ULK3 regulates the timing of membrane abscission, thus being involved in exosome budding and cytokinesis. Herein, we present the first high-resolution structures of the ULK3 kinase domain. Its unique features are explored against the background of other ULK kinases. An inhibitor fingerprint indicates that ULK3 is highly druggable and capable of adopting a wide range of conformations. In accordance with this, we describe a conformational switch between the active and an inactive ULK3 conformation, controlled by the properties of the attached small-molecule binder. Finally, we discuss a potential substrate-recognition mechanism of the full-length ULK3 protein.
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