Comparison of force fields to study the zinc-finger containing protein NPL4, a target for disulfiram in cancer therapy

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2023-07-01 DOI:10.1016/j.bbapap.2023.140921
Simone Scrima , Matteo Tiberti , Ulf Ryde , Matteo Lambrughi , Elena Papaleo
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引用次数: 1

Abstract

Molecular dynamics (MD) simulations are a powerful approach to studying the structure and dynamics of proteins related to health and disease. Advances in the MD field allow modeling proteins with high accuracy. However, modeling metal ions and their interactions with proteins is still challenging. NPL4 is a zinc-binding protein and works as a cofactor for p97 to regulate protein homeostasis. NPL4 is of biomedical importance and has been proposed as the target of disulfiram, a drug recently repurposed for cancer treatment. Experimental studies proposed that the disulfiram metabolites, bis-(diethyldithiocarbamate)‑copper and cupric ions, induce NPL4 misfolding and aggregation. However, the molecular details of their interactions with NPL4 and consequent structural effects are still elusive. Here, biomolecular simulations can help to shed light on the related structural details. To apply MD simulations to NPL4 and its interaction with copper the first important step is identifying a suitable force field to describe the protein in its zinc-bound states. We examined different sets of non-bonded parameters because we want to study the misfolding mechanism and cannot rule out that the zinc may detach from the protein during the process and copper replaces it. We investigated the force-field ability to model the coordination geometry of the metal ions by comparing the results from MD simulations with optimized geometries from quantum mechanics (QM) calculations using model systems of NPL4. Furthermore, we investigated the performance of a force field including bonded parameters to treat copper ions in NPL4 that we obtained based on QM calculations.

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比较力场研究含锌指蛋白NPL4,二硫仑在癌症治疗中的靶点
分子动力学(MD)模拟是研究与健康和疾病相关的蛋白质结构和动力学的有力方法。MD领域的进展使得能够高精度地对蛋白质进行建模。然而,对金属离子及其与蛋白质的相互作用进行建模仍然具有挑战性。NPL4是一种锌结合蛋白,作为p97的辅因子调节蛋白质稳态。NPL4具有生物医学重要性,已被提议作为双硫仑的靶点,双硫仑是一种最近重新用于癌症治疗的药物。实验研究表明,双硫仑代谢产物双(二乙基二硫代氨基甲酸酯)铜和铜离子会诱导NPL4错误折叠和聚集。然而,它们与NPL4相互作用的分子细节以及由此产生的结构效应仍然难以捉摸。在这里,生物分子模拟可以帮助阐明相关的结构细节。为了将MD模拟应用于NPL4及其与铜的相互作用,第一个重要步骤是确定合适的力场来描述处于锌结合状态的蛋白质。我们检查了不同的非键参数,因为我们想研究错误折叠机制,并且不能排除锌在这个过程中可能与蛋白质分离,而铜取代了它。我们通过将MD模拟的结果与使用NPL4模型系统的量子力学(QM)计算的优化几何结构进行比较,研究了对金属离子配位几何结构进行建模的力场能力。此外,我们研究了包括键合参数的力场的性能,以处理NPL4中的铜离子,这是我们基于QM计算获得的。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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