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首页> 外文期刊>The journal of physical chemistry, B. Condensed matter, materials, surfaces, interfaces & biophysical >Coarse-Grained Antibody Models for 'Weak' Protein-Protein Interactions from Low to High Concentrations
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Coarse-Grained Antibody Models for 'Weak' Protein-Protein Interactions from Low to High Concentrations

机译:从“低”到“高”浓度的“弱”蛋白质-蛋白质相互作用的粗粒抗体模型

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摘要

So-called "weak" protein-protein interactions are important for the control of solution properties and stability at elevated protein concentrations (c(2)) but are not practical to capture in atomistic simulations. This report a focuses on a series of coarse-grained models for predicting second osmotic virial coefficients (B-22) and high-concentration Rayleigh scattering (osmotic compressibility) as a function of c(2) for monoclonal antibodies (MAbs) that are of interest in biotechnology. B-22 and molecular volume along with c(2)-dependent osmotic compressibility were calculated for a series of models with increasing structural detail. Models were refined to include contributions from sterics, short-ranged van der Waals and hydrophobic attractions, screened electrostatics, and the flexibility of the mAb hinge region. The results highlight shortcomings for spherical models of MAbs and a useful balance between numerical accuracy and computational burden offered by models based on 6 or 12 spherical, partly overlapping domains. The results provide bounds for realistic values of effective charges on variable domains in order for MAbs to be stable in solution and more generally illustrate semiquantitative bounds for the space of model parameters that can reproduce experimental behavior and provide a basis for future development of computationally efficient and accurate CG mAb models to predict both low-and high-c(2) behavior.
机译:所谓的“弱”蛋白质-蛋白质相互作用对于控制溶液性质和在升高的蛋白质浓度下的稳定性很重要(c(2)),但在原子模拟中不实用。本报告重点介绍了一系列粗粒度模型,这些模型可预测单克隆抗体(MAb)的第二渗透病毒系数(B-22)和高浓度瑞利散射(渗透压缩性)与c(2)的关系。对生物技术的兴趣。 B-22和分子体积以及c(2)依赖的渗透性可压缩性为一系列增加结构细节的模型计算的。对模型进行了完善,以包括以下方面的贡献:空间位阻,短距离范德华力和疏水引力,筛选的静电以及mAb铰链区的柔性。结果突出了单克隆抗体的球形模型的缺点,以及基于6或12个球形,部分重叠的球形模型提供的数值精度和计算负担之间的有效平衡。结果为可变域上有效电荷的实际值提供了界线,以便使单克隆抗体在溶液中稳定,并且更普遍地说明了模型参数空间的半定量界线,可以再现实验行为,并为将来开发高效计算和计算提供基础。准确的CG mAb模型可预测低c(2)和高c(2)行为。

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