Advancing Membrane-Associated Protein Docking with Improved Sampling and Scoring in Rosetta.

IF 5.7 1区化学 Q2 CHEMISTRY, PHYSICAL

Journal of Chemical Theory and Computation Pub Date : 2024-11-22 DOI:10.1021/acs.jctc.4c00927

Rituparna Samanta, Ameya Harmalkar, Priyamvada Prathima, Jeffrey J Gray

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引用次数: 0

Abstract

The oligomerization of protein macromolecules on cell membranes plays a fundamental role in regulating cellular function. From modulating signal transduction to directing immune response, membrane proteins (MPs) play a crucial role in biological processes and are often the target of many pharmaceutical drugs. Despite their biological relevance, the challenges in experimental determination have hampered the structural availability of membrane proteins and their complexes. Computational docking provides a promising alternative to model membrane protein complex structures. Here, we present Rosetta-MPDock, a flexible transmembrane (TM) protein docking protocol that captures binding-induced conformational changes. Rosetta-MPDock samples large conformational ensembles of flexible monomers and docks them within an implicit membrane environment. We benchmarked this method on 29 TM-protein complexes of variable backbone flexibility. These complexes are classified based on the root-mean-square deviation between the unbound and bound states (RMSD_UB) as rigid (RMSD_UB < 1.2 Å), moderately flexible (RMSD_UB ∈ [1.2, 2.2] Å), and flexible targets (RMSD_UB > 2.2 Å). In a local docking scenario, i.e. with membrane protein partners starting ≈10 Å apart embedded in the membrane in their unbound conformations, Rosetta-MPDock successfully predicts the correct interface (success defined as achieving 3 near-native structures in the 5 top-ranked models) for 67% moderately flexible targets and 60% of the highly flexible targets, a substantial improvement from the existing membrane protein docking methods. Further, by integrating AlphaFold2-multimer for structure determination and using Rosetta-MPDock for docking and refinement, we demonstrate improved success rates over the benchmark targets from 64% to 73%. Rosetta-MPDock advances the capabilities for membrane protein complex structure prediction and modeling to tackle key biological questions and elucidate functional mechanisms in the membrane environment. The benchmark set and the code is available for public use at github.com/Graylab/MPDock.

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通过改进 Rosetta 中的采样和评分推进膜相关蛋白质对接

细胞膜上蛋白质大分子的寡聚化在调节细胞功能方面起着重要作用。从调节信号转导到引导免疫反应，膜蛋白（MPs）在生物过程中发挥着至关重要的作用，通常也是许多药物的靶标。尽管膜蛋白具有生物学相关性，但实验测定方面的挑战阻碍了膜蛋白及其复合物结构的可用性。计算对接为建立膜蛋白复合物结构模型提供了一种很有前景的替代方法。在这里，我们介绍了一种灵活的跨膜（TM）蛋白质对接方案 Rosetta-MPDock，它能捕捉结合引起的构象变化。Rosetta-MPDock 对柔性单体的大型构象组合进行采样，并在隐式膜环境中进行对接。我们在 29 个骨架柔性可变的 TM 蛋白复合物上对该方法进行了基准测试。这些复合物根据未结合态和结合态的均方根偏差（RMSDUB）分为刚性（RMSDUB < 1.2 Å）、中等柔性（RMSDUB ∈ [1.2, 2.2] Å）和柔性目标（RMSDUB > 2.2 Å）。在局部对接情况下，即膜蛋白伙伴以未结合构象嵌入膜中，开始时相距≈10 Å，Rosetta-MPDock 成功预测了 67% 的中度柔性目标物和 60% 的高度柔性目标物的正确界面（成功的定义是在 5 个排名靠前的模型中实现 3 个接近原生的结构），比现有的膜蛋白对接方法有了很大改进。此外，通过整合用于结构确定的 AlphaFold2-multimer，并使用 Rosetta-MPDock 进行对接和细化，我们证明与基准目标相比，成功率从 64% 提高到 73%。Rosetta-MPDock 提高了膜蛋白复合物结构预测和建模的能力，从而解决了关键的生物学问题，并阐明了膜环境中的功能机制。基准集和代码可在 github.com/Graylab/MPDock 上公开使用。

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来源期刊

Journal of Chemical Theory and Computation 化学-物理：原子、分子和化学物理

CiteScore

9.90

自引率

16.40%

发文量

568

审稿时长

1 months

期刊介绍： The Journal of Chemical Theory and Computation invites new and original contributions with the understanding that, if accepted, they will not be published elsewhere. Papers reporting new theories, methodology, and/or important applications in quantum electronic structure, molecular dynamics, and statistical mechanics are appropriate for submission to this Journal. Specific topics include advances in or applications of ab initio quantum mechanics, density functional theory, design and properties of new materials, surface science, Monte Carlo simulations, solvation models, QM/MM calculations, biomolecular structure prediction, and molecular dynamics in the broadest sense including gas-phase dynamics, ab initio dynamics, biomolecular dynamics, and protein folding. The Journal does not consider papers that are straightforward applications of known methods including DFT and molecular dynamics. The Journal favors submissions that include advances in theory or methodology with applications to compelling problems.