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用于测试肾小球滤过选择性的探针:Ficoll和右旋糖酐与球状蛋白的比较——分子大小、形状、电荷及可变形性的影响

Ficoll and dextran vs. globular proteins as probes for testing glomerular permselectivity: effects of molecular size, shape, charge, and deformability.

作者信息

Venturoli Daniele, Rippe Bengt

机构信息

Dept. of Nephrology, Univ. Hospital of Lund, S-211 85 Lund, Sweden.

出版信息

Am J Physiol Renal Physiol. 2005 Apr;288(4):F605-13. doi: 10.1152/ajprenal.00171.2004.

Abstract

Polydisperse mixtures of dextran or Ficoll have been frequently used as molecular probes for studies of glomerular permselectivity because they are largely inert and not processed (reabsorbed) by the proximal tubules. However, dextrans are linear, flexible molecules, which apparently are hyperpermeable across the glomerular barrier. By contrast, the Ficoll molecule is almost spherical. Still, there is ample evidence that Ficoll fractional clearances (sieving coefficients) across the glomerular capillary wall (GCW) are markedly higher than those for neutral globular proteins of an equivalent in vitro Stokes-Einstein (SE) radius. Physical data, obtained by "crowding" experiments or measurements of intrinsic viscosity, suggest that the Ficoll molecule exhibits a rather open, deformable structure and thus deviates from an ideally hard sphere. This is also indicated from the relationship between (log) in vitro SE radius and (log) molecular weight (MW). Whereas globular proteins seem to behave in a way similar to hydrated hard spheres, polydisperse dextran and Ficoll exhibit in vitro SE radii that are much larger than those for compact spherical molecules of equivalent MW. For dextran, this can be partially explained by a high-molecular-size asymmetry. However, for Ficoll the explanation may be that the Ficoll molecule is more flexible (deformable) than are globular proteins. An increased compressibility of Ficoll and an increased deformability and size asymmetry for dextran may be the explanation for the fact that the permeability of the GCW is significantly higher when assessed using polysaccharides such as Ficoll or dextran compared with that obtained using globular proteins as molecular size probes. We suggest that molecular deformability, besides molecular size, shape, and charge, plays a crucial role in determining the glomerular permeability to molecules of different species.

摘要

葡聚糖或聚蔗糖的多分散混合物经常被用作分子探针来研究肾小球滤过选择性,因为它们基本上是惰性的,不会被近端小管处理(重吸收)。然而,葡聚糖是线性的柔性分子,显然在肾小球屏障中具有高通透性。相比之下,聚蔗糖分子几乎是球形的。尽管如此,有充分的证据表明,聚蔗糖通过肾小球毛细血管壁(GCW)的分数清除率(筛滤系数)明显高于具有相同体外斯托克斯 - 爱因斯坦(SE)半径的中性球蛋白。通过“拥挤”实验或特性粘度测量获得的物理数据表明,聚蔗糖分子呈现出相当开放、可变形的结构,因此偏离了理想的硬球。这也从体外SE半径与分子量(MW)的(对数)关系中得到体现。球状蛋白的行为似乎类似于水合硬球,而多分散的葡聚糖和聚蔗糖的体外SE半径比同等MW的紧密球形分子的SE半径大得多。对于葡聚糖,这可以部分地由高分子尺寸不对称来解释。然而,对于聚蔗糖,解释可能是聚蔗糖分子比球状蛋白更具柔性(可变形)。聚蔗糖可压缩性的增加以及葡聚糖可变形性和尺寸不对称性的增加,可能是与使用球状蛋白作为分子大小探针相比,使用聚蔗糖或葡聚糖等多糖评估时GCW通透性显著更高这一事实的解释。我们认为,除了分子大小、形状和电荷外,分子可变形性在决定肾小球对不同种类分子的通透性方面起着关键作用。

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