Université Paris Descartes, Inserm U, CNRS UMR, UFR des Sciences Pharmaceutiques et Biologiques, France.
Proteins. 2010 May 1;78(6):1520-30. doi: 10.1002/prot.22669.
In a previous study, we identified 12 conserved domains within pUL89, the small terminase subunit of the human cytomegalovirus. A latter study showed that the fragment pUL89(580-600) plays an important role in the formation of the terminase complex by interacting with the large terminase subunit pUL56. In this study, analysis was performed to solve the structure of pUL89(568-635) in 50% H2O/50% acetonitrile (v/v). We showed that pUL89(568-635) consists of four alpha helices, but we did not identify any tertiary structure. The fragment 580-600 formed an amphipathic alpha helix, which had a hydrophobic side highly conserved among herpesviral homologs of pUL89; this was not observed for its hydrophilic side. The modeling of pUL89(457-612) using the recognition fold method allowed us to position pUL89(580-600) within this domain. The theoretical structure highlighted three important features. First, we identified a metal-binding pocket containing residues Asp(463), Glu(534), and Glu(588), which are highly conserved among pUL89 homologs. Second, the model predicted a positively charged surface able to interact with the DNA duplex during the nicking event. Third, a hydrophobic patch on the top of the catalytic site suggested that this may constitute part of the pUL89 site recognized by pUL56 potentially involved in DNA binding.
在之前的一项研究中,我们在人巨细胞病毒的小末端酶亚基 pUL89 中鉴定出 12 个保守结构域。后来的一项研究表明,片段 pUL89(580-600) 通过与大末端酶亚基 pUL56 相互作用,在末端酶复合物的形成中发挥重要作用。在这项研究中,我们进行了分析以解决在 50%H2O/50%乙腈(v/v)中 pUL89(568-635) 的结构。我们表明 pUL89(568-635) 由四个α螺旋组成,但我们没有鉴定出任何三级结构。片段 580-600 形成一个两亲性α螺旋,其疏水侧在疱疹病毒 pUL89 同源物中高度保守;亲水侧则没有。使用识别折叠方法对 pUL89(457-612) 进行建模,使我们能够将 pUL89(580-600) 定位在该结构域内。理论结构突出了三个重要特征。首先,我们鉴定出一个含有残基 Asp(463)、Glu(534)和 Glu(588)的金属结合口袋,这些残基在 pUL89 同源物中高度保守。其次,该模型预测了一个带正电荷的表面,能够在切口事件中与 DNA 双链相互作用。第三,催化位点顶部的一个疏水区表明,这可能构成被 pUL56 识别的 pUL89 位点的一部分,可能参与 DNA 结合。
