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L-选择素与碳水化合物的相互作用:Lewis x三糖的相关修饰

L-selectin-carbohydrate interactions: relevant modifications of the Lewis x trisaccharide.

作者信息

Sanders W J, Katsumoto T R, Bertozzi C R, Rosen S D, Kiessling L L

机构信息

Department of Chemistry, University of Wisconsin, Madison 53706, USA.

出版信息

Biochemistry. 1996 Nov 26;35(47):14862-7. doi: 10.1021/bi9613640.

DOI:10.1021/bi9613640
PMID:8942649
Abstract

Protein-carbohydrate interactions are known to mediate cell-cell recognition and adhesion events. Specifically, three carbohydrate binding proteins termed selectins (E-, P-, and L-selectin) have been shown to be essential for leukocyte rolling along the vascular endothelium, the first step in the recruitment of leukocytes from the blood into inflammatory sites or into secondary lymphoid organs. Although this phenomenon is well-established, little is known about the molecular-level interactions on which it depends. All three selectins recognize sulfated and sialylated derivatives of the Lewis x [Le(x):Gal beta 1-->4(Fuc alpha 1-->3)GlcNAc] and Lewis a [Le(a): Gal beta 1-->3(Fuc alpha 1-->4)GlcNAc] trisaccharide cores with affinities in the millimolar range, and it is believed that variants of these structures are the carbohydrate determinants of selectin recognition. Recently it was shown that the mucin GlyCAM-1, a secreted physiological ligand for L-selectin, is capped with sulfated derivatives of sialyl Lewis x [sLe(x): Sia alpha 2-->3Gal beta 1-->4(Fuc alpha 1-->3)GlcNAc] and that sulfation is required for the high-affinity interaction between GlyCAM-1 and L-selectin. To elucidate the important sites of sulfation on Le(x) with respect to L-selectin recognition, we have synthesized six sulfated Le(x) analogs and determined their abilities to block binding of a recombinant L-selectin-Ig chimera to immobilized GlyCAM-1. Our results suggest that 6-sulfo sLe(x) binds to L-selectin with higher affinity than does sLe(x) or 6'-sulfo sLe(x) and that sulfation of sLe(x) capping groups on GlyCAM-1 at the 6-position is important for L-selectin recognition.

摘要

已知蛋白质 - 碳水化合物相互作用介导细胞间识别和黏附事件。具体而言,三种被称为选择素(E - 选择素、P - 选择素和L - 选择素)的碳水化合物结合蛋白已被证明对于白细胞沿血管内皮滚动至关重要,这是白细胞从血液募集到炎症部位或二级淋巴器官的第一步。尽管这一现象已得到充分证实,但对于其依赖的分子水平相互作用却知之甚少。所有三种选择素都能识别具有毫摩尔级亲和力的Lewis x [Le(x):Galβ1→4(Fucα1→3)GlcNAc]和Lewis a [Le(a):Galβ1→3(Fucα1→4)GlcNAc]三糖核心的硫酸化和唾液酸化衍生物,并且据信这些结构的变体是选择素识别的碳水化合物决定簇。最近有研究表明,黏蛋白GlyCAM - 1是L - 选择素的一种分泌型生理配体,其被唾液酸化Lewis x [sLe(x):Siaα2→3Galβ1→4(Fucα1→3)GlcNAc]的硫酸化衍生物所覆盖,并且硫酸化是GlyCAM - 1与L - 选择素之间高亲和力相互作用所必需的。为了阐明相对于L - 选择素识别而言Le(x)上硫酸化的重要位点,我们合成了六种硫酸化的Le(x)类似物,并确定了它们阻断重组L - 选择素 - Ig嵌合体与固定化GlyCAM - 1结合的能力。我们的结果表明,6 - 磺基sLe(x)与L - 选择素结合的亲和力高于sLe(x)或6'- 磺基sLe(x),并且GlyCAM - 1上sLe(x)封端基团在6位的硫酸化对于L - 选择素识别很重要。

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