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The crystal structure of the human polo-like kinase-1 polo box domain and its phospho-peptide complex

机译:人polo样激酶1 polo框结构域的晶体结构及其磷酸肽复合物

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摘要

Human polo-like kinase Plk1 localizes to the centrosomes, kinetochores and central spindle structures during mitosis. It plays an essential role in promoting mitosis and cytokinesis through phosphorylation of a number of different substrates. Kinase activity is regulated by a conserved C-terminal domain, termed the polo box domain (PBD), which acts both as an autoinhibitory domain and as a subcellular localization domain. We have determined the crystal structure of Plk1 PBD (residues 367–603) to 2.2 Å resolution and the structure of a phospho-peptide–PBD (residues 345–603) complex to 2.3 Å resolution. The two polo boxes of the PBD exhibit identical folds based on a six-stranded β-sheet and an α-helix, despite only 12% sequence identity. The phospho-peptide binds at a site between the two polo boxes. It makes a short antiparallel β-sheet connection and critical contacts to residues Trp414, Leu490, His538 and Lys540. Most of these residues had been shown to be important for biological activity through mutational studies. The results provide an explanation for phospho-peptide recognition and create the basis for new functional studies.
机译:人类的马球样激酶Plk1在有丝分裂过程中定位于中心体,动植物和中心纺锤体结构。它通过许多不同底物的磷酸化在促进有丝分裂和胞质分裂中起重要作用。激酶活性由保守的C端结构域调节,该结构域称为polo框结构域(PBD),其既充当自抑制域又充当亚细胞定位域。我们确定了Plk1 PBD(残基367–603)的晶体结构达到2.2的分辨率,以及磷酸肽–PBD(残基345–603)复杂的晶体结构至2.3的分辨率。尽管只有12%的序列同一性,但PBD的两个polo盒基于六链β-折叠和α-螺旋显示出相同的折叠。磷酸肽结合在两个马球盒之间的位点。它可以短的反平行β-折叠连接和与残基Trp414,Leu490,His538和Lys540的关键接触。通过突变研究表明,这些残基中的大多数对生物学活性均很重要。结果为磷酸肽识别提供了解释,并为新的功能研究奠定了基础。

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