{"title":"噬菌体 P22 N 肽与 BoxB RNA 的耦合折叠和结合的高级取样模拟。","authors":"Luis Vollmers, Martin Zacharias","doi":"10.1016/j.bpj.2024.08.022","DOIUrl":null,"url":null,"abstract":"<p><p>Protein-RNA interactions are crucially important for numerous cellular processes and often involve coupled folding and binding of peptide segments upon association. The Nut-utilization site (N)-protein of bacteriophages contains an N-terminal arginine-rich motif that undergoes such a folding transition upon binding to the boxB RNA hairpin loop target structure. Molecular dynamics free energy simulations were used to calculate the absolute binding free energy of the N-peptide of bacteriophage P22 in complex with the boxB RNA hairpin motif at different salt concentrations and using two different water force field models. We obtained good agreement with experiment also at different salt concentrations for the TIP4P-D water model that has a stabilizing effect on unfolded protein structures. It allowed us to estimate the free energy contribution resulting from restricting the molecules' spatial and conformational freedom upon binding, which makes a large opposing contribution to binding. In a second set of umbrella sampling simulations to dissociate/associate the complex along a separation coordinate, we analyzed the onset of preorientation of the N-peptide and onset of structure formation relative to the RNA and its dependence on the salt concentration. Peptide orientation and conformational transitions are significantly coupled to the first contact formation between peptide and RNA. The initial contacts are mostly formed between peptide residues and the boxB hairpin loop nucleotides. A complete transition to an α-helical bound peptide conformation occurs only at a late stage of the binding process a few angstroms before the complexed state has been reached. However, the N-peptide orients also at distances beyond the contact distance such that the sizable positive charge points toward the RNA's center-of-mass. 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In a second set of umbrella sampling simulations to dissociate/associate the complex along a separation coordinate, we analyzed the onset of preorientation of the N-peptide and onset of structure formation relative to the RNA and its dependence on the salt concentration. Peptide orientation and conformational transitions are significantly coupled to the first contact formation between peptide and RNA. The initial contacts are mostly formed between peptide residues and the boxB hairpin loop nucleotides. A complete transition to an α-helical bound peptide conformation occurs only at a late stage of the binding process a few angstroms before the complexed state has been reached. However, the N-peptide orients also at distances beyond the contact distance such that the sizable positive charge points toward the RNA's center-of-mass. 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引用次数: 0
摘要
蛋白质与 RNA 的相互作用对许多细胞过程都至关重要,而且往往涉及肽段在结合时的耦合折叠和结合。噬菌体的坚果利用位点(N)蛋白含有一个 N 端富含精氨酸的基团,在与 boxB RNA 发夹环目标结构结合时会发生这种折叠转变。我们利用分子动力学(MD)自由能模拟计算了噬菌体 P22 的 N 肽在不同盐浓度下与 boxB RNA 发夹图案复合时的绝对结合自由能,并使用了两种不同的水力场模型。在不同盐浓度条件下,我们发现 TIP4P-D 水模型与实验结果的一致性很好,该模型对未折叠蛋白质结构具有稳定作用。这使我们能够估算出在结合时限制分子的空间和构象自由度所产生的自由能贡献,这对结合有很大的反作用。在第二组伞状取样模拟中,我们沿分离坐标解离/分离了复合物,分析了 N 肽预取向的开始时间和相对于 RNA 的结构形成的开始时间及其对盐浓度的依赖性。肽的取向和构象转变与肽和 RNA 之间首次接触的形成密切相关。最初的接触主要是在多肽残基与 boxB 发夹环核苷酸之间形成的。只有在结合过程的晚期,即达到复合状态之前几埃处,才会完全转变为α螺旋结合肽构象。然而,N-肽也会在接触距离以外的地方定向,从而使相当大的正电荷指向 RNA 的质量中心。我们的研究结果可能对理解经常涉及耦合折叠和结合过程的蛋白质和肽-RNA复合物的形成具有重要意义。
Advanced sampling simulations of coupled folding and binding of phage P22 N-peptide to boxB RNA.
Protein-RNA interactions are crucially important for numerous cellular processes and often involve coupled folding and binding of peptide segments upon association. The Nut-utilization site (N)-protein of bacteriophages contains an N-terminal arginine-rich motif that undergoes such a folding transition upon binding to the boxB RNA hairpin loop target structure. Molecular dynamics free energy simulations were used to calculate the absolute binding free energy of the N-peptide of bacteriophage P22 in complex with the boxB RNA hairpin motif at different salt concentrations and using two different water force field models. We obtained good agreement with experiment also at different salt concentrations for the TIP4P-D water model that has a stabilizing effect on unfolded protein structures. It allowed us to estimate the free energy contribution resulting from restricting the molecules' spatial and conformational freedom upon binding, which makes a large opposing contribution to binding. In a second set of umbrella sampling simulations to dissociate/associate the complex along a separation coordinate, we analyzed the onset of preorientation of the N-peptide and onset of structure formation relative to the RNA and its dependence on the salt concentration. Peptide orientation and conformational transitions are significantly coupled to the first contact formation between peptide and RNA. The initial contacts are mostly formed between peptide residues and the boxB hairpin loop nucleotides. A complete transition to an α-helical bound peptide conformation occurs only at a late stage of the binding process a few angstroms before the complexed state has been reached. However, the N-peptide orients also at distances beyond the contact distance such that the sizable positive charge points toward the RNA's center-of-mass. Our result may have important implications for understanding protein- and peptide-RNA complex formation frequently involving coupled folding and association processes.
期刊介绍:
BJ publishes original articles, letters, and perspectives on important problems in modern biophysics. The papers should be written so as to be of interest to a broad community of biophysicists. BJ welcomes experimental studies that employ quantitative physical approaches for the study of biological systems, including or spanning scales from molecule to whole organism. Experimental studies of a purely descriptive or phenomenological nature, with no theoretical or mechanistic underpinning, are not appropriate for publication in BJ. Theoretical studies should offer new insights into the understanding ofexperimental results or suggest new experimentally testable hypotheses. Articles reporting significant methodological or technological advances, which have potential to open new areas of biophysical investigation, are also suitable for publication in BJ. Papers describing improvements in accuracy or speed of existing methods or extra detail within methods described previously are not suitable for BJ.
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