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Quantifying rolling adhesion with a cell-free assay: E-selectin and its carbohydrate ligands.

机译:用无细胞测定法定量滚动粘附:E-选择素及其碳水化合物配体。

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摘要

Rolling of neutrophils over stimulated endothelial cells is a prerequisite to firm attachment and subsequent transendothelial migration during the inflammatory response. The selectin family of adhesion molecules are thought to mediate rolling by binding counter-receptors that present carbohydrates, such as sialyl Lewis(x) (sLe[x]). Recently we described a cell-free system for rolling using sLe(x)-coated microspheres and E-selectin molecules on inert substrates. We showed that sLe(x)-coated microspheres rolled over E-selectin-IgG chimera substrates with dynamics that are similar to those of leukocytes rolling over stimulated endothelium. In this paper we provide a thorough quantitative description of the dynamics of adhesion for this system. We find that particle rolling velocity increases with increasing wall shear stress and decreases with increasing E-selectin or sLe(x) surface densities. Large changes in the average rolling velocity can occur with small changes in sLe(x) or E-selectin density; however, rolling velocity is more sensitive to E-selectin surface coverage than to the number of sLe(x) molecules on the microspheres. Aided by dimensional analysis, we show that decreasing the wall shear stress or increasing either receptor (E-selectin) or ligand (sLe[x]) surface coverage results in an equivalent decrease in particle rolling velocity. In addition, we find that different Lewis carbohydrates are more effective in mediating rolling on E-selectin, with effectiveness following the trend sialyl Lewis(a) > sialyl Lewis(x) >> sulfated Lewis(x) >> Lewis(x). Rolling velocity fluctuated with time for all carbohydrate-selectin pairs tested, and the magnitude of the velocity fluctuations was linearly proportional to the mean rolling velocity for all combinations of E-selectin site density, sLe(x) site density, wall shear stress, and carbohydrate chemistry tested.
机译:中性粒细胞在刺激的内皮细胞上滚动是炎症反应期间牢固附着和随后跨内皮迁移的先决条件。粘附分子的选择素家族被认为通过结合呈递碳水化合物的反受体例如唾液酸化的Lewis(x)(sLe [x])来介导滚动。最近,我们描述了一种无细胞系统,用于在惰性基质上使用sLe(x)涂层微球和E-选择素分子滚动。我们显示,sLe(x)涂层的微球在E-选择素IgG嵌合底物上滚动,其动力学类似于白细胞在刺激的内皮上滚动。在本文中,我们提供了对该系统粘附动力学的全面定量描述。我们发现,颗粒滚动速度随着壁切应力的增加而增加,而随着E-选择素或sLe(x)表面密度的增加而减小。 sLe(x)或E-选择素密度的较小变化可能会导致平均轧制速度发生较大变化。但是,滚动速度对E-选择素的表面覆盖比对微球上sLe(x)分子的数量更敏感。在尺寸分析的帮助下,我们表明降低壁切应力或增加受体(E-选择素)或配体(sLe [x])的表面覆盖率会导致等效的颗粒滚动速度降低。此外,我们发现不同的Lewis碳水化合物在介导E-选择素上的滚动更有效,其效仿趋势是唾液酸化Lewis(a)>唾液酸化Lewis(x)硫酸化Lewis(x) Lewis(x)。对于所有测试的碳水化合物选择素对,轧制速度均随时间波动,并且速度波动的大小与E选择素位点密度,sLe(x)位点密度,壁切应力和碳水化合物化学测试。

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