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Analysis of CD44-hyaluronan interactions in an artificial membrane system: Insights into the distinct binding properties of high and low molecular weight hyaluronan

机译:人工膜系统中CD44-透明质酸相互作用的分析:对高分子量和低分子量透明质酸的独特结合特性的见解

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摘要

CD44 is a major cell surface receptor for the large polydisperse glycosaminoglycan hyaluronan (HA). Binding of the long and flexible HA chains is thought to be stabilized by the multivalent nature of the sugar molecule. In addition, high and low molecular weight forms of HA provoke distinct proinflammatory and anti-inflammatory effects upon binding to CD44 and can deliver either proliferative or antiproliferative signals in appropriate cell types. Despite the importance of such interactions, however, neither the stoichiometry of multivalent HA binding at the cell surface nor the molecular basis for functional distinction between different HA size categories is understood. Here we report on the design of a supported lipid bilayer system that permits quantitative analysis of multivalent binding through presentation of CD44 in a stable, natively oriented manner and at controlled density. Using this system in combination with biophysical techniques, we show that the amount of HA binding to bilayers that are densely coated with CD44 increases as a function of HA size, with half-maximal saturation at ∼30 kDa. Moreover, reversible binding was confined to the smaller HA species (molecular weight of ≤10 kDa), whereas the interaction was essentially irreversible with larger polymers. The amount of bound HA decreased with decreasing receptor surface density, but the stability of binding was not affected. From a physico-chemical perspective, the binding properties of HA share many similarities with the typical behavior of a flexible polymer as it adsorbs onto a homogeneously attractive surface. These findings provide new insight into the multivalent nature of CD44-HA interactions and suggest a molecular basis for the distinct biological properties of different size fractions of hyaluronan. © 2010 by The American Society for Biochemistry and Molecular Biology, Inc.
机译:CD44是大型多分散糖胺聚糖透明质酸(HA)的主要细胞表面受体。糖分子的多价性质使长而柔韧的HA链的结合得以稳定。此外,高分子量和低分子量形式的HA在与CD44结合时会引起明显的促炎和抗炎作用,并且可以在适当的细胞类型中传递增殖或抗增殖信号。尽管这种相互作用很重要,但是,无论是在细胞表面结合多价HA的化学计量还是在不同HA大小类别之间进行功能区分的分子基础都无法理解。在这里,我们报告了支持的脂质双层系统的设计,该系统允许通过以稳定,天然定向的方式并以受控的密度呈递CD44来定量分析多价结合。通过将该系统与生物物理技术结合使用,我们显示出HA结合到被CD44密集包被的双层上的数量随HA尺寸的增加而增加,最大饱和度为〜30 kDa。此外,可逆结合仅限于较小的HA种类(分子量≤10kDa),而相互作用基本上与较大的聚合物不可逆。 HA的结合量随受体表面密度的降低而降低,但结合的稳定性并未受到影响。从理化角度看,HA的结合特性与柔性聚合物的典型行为有着很多相似之处,因为它吸附在均匀吸引的表面上。这些发现提供了对CD44-HA相互作用的多价性质的新见解,并为透明质酸不同大小级分的不同生物学特性提供了分子基础。 ©2010美国生物化学与分子生物学学会版权所有。

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