Department of Biochemistry, Duke University Medical Center, Durham, NC 27710, USA.
Biochemistry. 2010 Nov 9;49(44):9428-37. doi: 10.1021/bi100287y.
Protein folding intermediates are often imperative for overall folding processes and consequent biological functions. However, the low population and transient nature of the intermediate states often hinder their biochemical and biophysical characterization. Previous studies have demonstrated that Bacillus subtilis ribonuclease P protein (P protein) is conformationally heterogeneous and folds with multiphasic kinetics, indicating the presence of an equilibrium and kinetic intermediate in its folding mechanism. In this study, nuclear magnetic resonance (NMR) spectroscopy was used to study the ensemble corresponding to this intermediate (I). The results indicate that the N-terminal and C-terminal helical regions are mostly unfolded in I. 1H−15N heteronuclear single-quantum coherence NMR spectra collected as a function of pH suggest that the protonation of His 22 may play a major role in the energetics of the equilibria among the unfolded, intermediate, and folded state ensembles of P protein. NMR paramagnetic relaxation enhancement experiments were also used to locate the small anion binding sites in both the intermediate and folded ensembles. The results for the folded protein are consistent with the previously modeled binding regions. These structural insights suggest a possible role for I in the RNase P holoenzyme assembly process.
蛋白质折叠中间体对于整体折叠过程和后续的生物功能至关重要。然而,中间状态的低丰度和瞬态性质常常阻碍了它们的生化和生物物理特性的研究。先前的研究表明,枯草芽孢杆菌核糖核酸酶 P 蛋白(P 蛋白)构象异构,并且折叠具有多相动力学,这表明其折叠机制中存在平衡和动力学中间态。在这项研究中,使用核磁共振(NMR)光谱学来研究该中间态(I)的集合。结果表明,I 中 N 端和 C 端螺旋区大部分未折叠。随着 pH 值变化收集的 1H−15N 异核单量子相干 NMR 光谱表明,His22 的质子化可能在 P 蛋白未折叠、中间和折叠状态集合体之间的平衡能学中起主要作用。NMR 顺磁弛豫增强实验也用于定位中间态和折叠态集合体中的小阴离子结合位点。折叠蛋白的结果与先前建模的结合区域一致。这些结构见解表明 I 可能在 RNase P 全酶组装过程中发挥作用。