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金黄色葡萄球菌中细菌细胞分裂蛋白FtsZ的结构重组

Structural reorganization of the bacterial cell-division protein FtsZ from Staphylococcus aureus.

作者信息

Matsui Takashi, Yamane Junji, Mogi Nobuyuki, Yamaguchi Hiroto, Takemoto Hiroshi, Yao Min, Tanaka Isao

机构信息

Faculty of Advanced Life Science, Hokkaido University, Sapporo, Hokkaido, Japan.

出版信息

Acta Crystallogr D Biol Crystallogr. 2012 Sep;68(Pt 9):1175-88. doi: 10.1107/S0907444912022640. Epub 2012 Aug 18.

Abstract

FtsZ is a key molecule in bacterial cell division. In the presence of GTP, it polymerizes into tubulin-like protofilaments by head-to-tail association. Protofilaments of FtsZ seem to adopt a straight or a curved conformation in relation to the bound nucleotide. However, although several bacterial and archaeal FtsZ structures have been determined, all of the structures reported previously are considered to have a curved conformation. In this study, structures of FtsZ from Staphylococcus aureus (SaFtsZ) were determined in apo, GDP-bound and inhibitor-complex forms and it was found that SaFtsZ undergoes marked conformational changes. The accumulated evidence suggests that the GDP-bound structure has the features of the straight form. The structural change between the curved and straight forms shows intriguing similarity to the eukaryotic cytoskeletal protein tubulin. Furthermore, the structure of the apo form showed an unexpectedly large conformational change in the core region. FtsZ has also been recognized as a novel target for antibacterial drugs. The structure of the complex with the inhibitor PC190723, which has potent and selective antistaphylococcal activity, indicated that the inhibitor binds at the cleft between the two subdomains.

摘要

FtsZ是细菌细胞分裂中的关键分子。在GTP存在的情况下,它通过头对头结合聚合成微管蛋白样原丝。FtsZ原丝相对于结合的核苷酸似乎呈现出直线或弯曲构象。然而,尽管已经确定了几种细菌和古细菌的FtsZ结构,但之前报道的所有结构都被认为具有弯曲构象。在本研究中,测定了金黄色葡萄球菌FtsZ(SaFtsZ)的无配体、结合GDP和抑制剂复合物形式的结构,发现SaFtsZ经历了显著的构象变化。累积的证据表明,结合GDP的结构具有直线形式的特征。弯曲形式和直线形式之间的结构变化与真核细胞骨架蛋白微管蛋白具有有趣的相似性。此外,无配体形式的结构在核心区域显示出意外的大构象变化。FtsZ也被认为是抗菌药物的新靶点。与具有强大和选择性抗葡萄球菌活性的抑制剂PC190723形成的复合物结构表明,该抑制剂结合在两个亚结构域之间的裂隙处。

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