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Properties of DNA- and Protein-Scaffolded Lipid Nanodiscs

机译:DNA和蛋白质 - 脚手架脂质纳米DISC的性质

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摘要

The properties of natural lipid bilayers are vital to the regulation of many membrane proteins. Scaffolded nanodiscs provide an in vitro lipid bilayer platform to host membrane proteins in an environment that approximates native lipid bilayers. However, the properties of scaffold-enclosed bilayers may depart significantly from those of bulk cellular membranes. Therefore, to improve the usefulness of nanodiscs it is essential to understand the properties of lipids restricted by scaffolds. We used computational molecular dynamics and modeling approaches to understand the effects of nanodisc size, scaffold type (DNA or protein), and hydrophobic modification of DNA scaffolds on bilayer stability and degree to which the properties of enclosed bilayers approximate bulk bilayers. With respect to achieving bulk bilayer behavior, we found that charge neutralization of DNA scaffolds was more important than the total hydrophobic content of their modifications: bilayer properties were better for scaffolds having a large number of short alkyl chains than those having fewer long alkyl chains. Further, complete charge neutralization of DNA scaffolds enabled better lipid binding, and more stable bilayers, as shown by steered molecular dynamics simulations that measured the force required to dislodge scaffolds from lipid bilayer patches. Considered together, our simulations provide a guide to the design of DNA-scaffolded nanodiscs suitable for studying membrane proteins.
机译:天然脂质双层的性质对许多膜蛋白的调节至关重要。支架纳米盘提供了一个体外脂质双层平台,在接近天然脂质双层的环境中宿主膜蛋白。然而,支架封闭双层膜的性能可能与体细胞膜的性能显著不同。因此,为了提高纳米盘的实用性,有必要了解受支架限制的脂质的性质。我们使用计算分子动力学和建模方法来理解纳米盘大小、支架类型(DNA或蛋白质)和DNA支架的疏水性修饰对双层稳定性的影响,以及封闭双层的性质接近大块双层的程度。关于实现大块双层行为,我们发现DNA支架的电荷中和比其修饰的总疏水含量更重要:具有大量短烷基链的支架的双层性能优于具有较少长烷基链的支架。此外,DNA支架的完全电荷中和能够实现更好的脂质结合和更稳定的双层,如定向分子动力学模拟所示,该模拟测量了将支架从脂质双层贴片上移除所需的力。综合考虑,我们的模拟为设计适合研究膜蛋白的DNA支架纳米盘提供了指导。

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