论文标题

单分散样品的小角度X射线散射实验接近溶解度极限

Small angle x-ray scattering experiments of monodisperse samples close to the solubility limit

论文作者

Martin, Erik W., Hopkins, Jesse B., Mittag, Tanja

论文摘要

生物分子通过液态液相分离(LLP)将生物分子缩合到生物分子冷凝物中,是一种驱动细胞组织的无处不在的机制。为了启用这些功能,生物分子已经进化为驱动LLP并促进分配成生物分子冷凝物。确定编码LLP的蛋白质的分子特征将为许多生物过程提供关键的见解。在问题上,直接探测生物分子密集阶段通常是技术困难或不可能的。通过利用稀释溶液和致密相中生物分子的构象行为之间的对称性,可以通过精确测量稀阶段的精确测量来推断对相分离至关重要的细节,从而避免了密集相的复杂表征。稀释和致密相之间的对称性以生物分子的构象合奏的大小和形状 - 小角度X射线散射(SAX)的参数非常适合探测。最近的技术进步使得能够准确地表征足够低浓度的固有无序蛋白质区域样品,以避免从分子间吸引,低聚或聚集中干扰,这些样本以前所有这些以前都是障碍,以表征自组装蛋白的表征。在本文中,我们描述了测量此类样本固有的陷阱,规避这些问题所需的细节以及将SAXS测量结果置于LLP的理论框架中的分析方法。

The condensation of biomolecules into biomolecular condensates via liquid-liquid phase separation (LLPS) is a ubiquitous mechanism that drives cellular organization. To enable these functions, biomolecules have evolved to drive LLPS and facilitate partitioning into biomolecular condensates. Determining the molecular features of proteins that encode LLPS will provide critical insights into a plethora of biological processes. Problematically, probing biomolecular dense phases directly is often technologically difficult or impossible. By capitalizing on the symmetry between the conformational behavior of biomolecules in dilute solution and dense phases, it is possible to infer details critical to phase separation by precise measurements of the dilute phase thus circumventing complicated characterization of dense phases. The symmetry between dilute and dense phases is found in the size and shape of the conformational ensemble of a biomolecule - parameters that small-angle x-ray scattering (SAXS) is ideally suited to probe. Recent technological advances have made it possible to accurately characterize samples of intrinsically disordered protein regions at low enough concentration to avoid interference from intermolecular attraction, oligomerization or aggregation, all of which were previously roadblocks to characterizing self-assembling proteins. Herein, we describe the pitfalls inherent to measuring such samples, the details required for circumventing these issues and analysis methods that place the results of SAXS measurements into the theoretical framework of LLPS.

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