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Endoglycan, a Member of the CD34 Family of Sialomucins, Is a Ligand for the Vascular Selectins

机译:内糖是唾液粘蛋白​​CD34家族的成员,是血管选择素的配体。

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The interactions of the selectin family of adhesion molecules with their ligands are essential for the initial rolling stage of leukocyte trafficking. Under inflammatory conditions, the vascular selectins, E- and P-selectin, are expressed on activated vessels and interact with carbohydrate-based ligands on the leukocyte surface. While several ligands have been characterized on human T cells, monocytes and neutrophils, there is limited information concerning ligands on B cells. Endoglycan (EG) together with CD34 and podocalyxin comprise the CD34 family of sialomucins. We found that EG, previously implicated as an L-selectin ligand on endothelial cells, was present on human B cells, T cells and peripheral blood monocytes. Upon activation of B cells, EG increased with a concurrent decrease in PSGL-1. Expression of EG on T cells remained constant under the same conditions. We further found that native EG from several sources (a B cell line, a monocyte line and human tonsils) was reactive with HECA-452, a mAb that recognizes sialyl Lewis X and related structures. Moreover, immunopurified EG from these sources was able to bind to P-selectin and where tested E-selectin. This interaction was divalent cation-dependent and required sialylation of EG. Finally, an EG construct supported slow rolling of E- and P-selectin bearing cells in a sialic acid and fucose dependent manner, and the introduction of intact EG into a B cell line facilitated rolling interactions on a P-selectin substratum. These in vitro findings indicate that EG can function as a ligand for the vascular selectins.
机译:选择素家族粘附分子与其配体的相互作用对于白细胞运输的初始滚动阶段是必不可少的。在炎症条件下,血管选择素E和P选择素在活化血管上表达,并与白细胞表面上基于碳水化合物的配体相互作用。尽管已经在人T细胞,单核细胞和嗜中性粒细胞上鉴定了几种配体,但有关B细胞上配体的信息有限。内糖(EG)与CD34和Podocalyxin一起构成唾液酸蛋白CD34家族。我们发现,以前与内皮细胞上的L-选择蛋白配体有关的EG存在于人B细胞,T细胞和外周血单核细胞上。 B细胞活化后,EG升高,同时PSGL-1降低。在相同条件下,EG在T细胞上的表达保持恒定。我们进一步发现,来自几种来源(B细胞系,单核细胞系和人扁桃体)的天然EG与HECA-452(识别唾液酸路易斯X和相关结构的mAb)有反应。此外,来自这些来源的免疫纯化的EG能够与P-选择素结合,并与受试的E-选择素结合。这种相互作用是二价阳离子依赖性的,并且需要EG的唾液酸化。最后,EG构建体以唾液酸和岩藻糖依赖性方式支持携带E-和P-选择蛋白的细胞缓慢滚动,并且将完整的EG引入B细胞系促进了P-选择蛋白基质上的滚动相互作用。这些体外发现表明,EG可以充当血管选择素的配体。

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