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P选择素和E选择素。不同但重叠的白细胞配体特异性。

P-selectin and E-selectin. Distinct but overlapping leukocyte ligand specificities.

作者信息

Larsen G R, Sako D, Ahern T J, Shaffer M, Erban J, Sajer S A, Gibson R M, Wagner D D, Furie B C, Furie B

机构信息

Genetics Institute Inc., Cambridge, Massachusetts 02140.

出版信息

J Biol Chem. 1992 Jun 5;267(16):11104-10.

PMID:1375936
Abstract

P-selectin on platelets and endothelial cells and E-selectin on endothelial cells are leukocyte receptors that recognize lineage-specific carbohydrates on neutrophils and monocytes. The proposed ligands for these receptors contain the Le(x) core and sialic acid. Since other investigators have shown that both E-selectin and P-selectin bind to sialylated Le(x), we evaluated whether E-selectin and P-selectin recognize the same counter-receptor on leukocytes. The interaction of HL60 cells with Chinese hamster ovary (CHO) cells expressing P-selectin or E-selectin was studied. To determine whether a protein component is required in addition to sialyl Le(x) for either P-selectin or E-selectin recognition, HL60 cells or neutrophils were digested with proteases, including chymotrypsin, elastase, proteinase Glu-C, ficin, papain, or thermolysin. Cells treated with these proteases bound E-selectin but not P-selectin. Fucosidase or neuraminidase treatment of HL60 cells markedly decreased binding to both E-selectin- and P-selectin-expressing CHO cells. Growth of HL60 cells in tunicamycin inhibited the ability of these cells to support P-selectin-mediated binding and, to a lesser extent, E-selectin-mediated binding. Purified P-selectin inhibited CHO:P-selectin binding to HL60 cells, but incompletely inhibited CHO:E-selectin binding to HL60 cells. However, purified soluble E-selectin inhibited CHO:P-selectin and CHO:E-selectin binding to HL60 cells equivalently and completely. COS cells, unable to bind to E-selectin or P-selectin, bound E-selectin but not P-selectin upon transfection with alpha-1,3-fucosyltransferase or alpha-1,3/1,4-fucosyltransferase. Similarly, LEC 11 cells expressing sialyl Le(x) bound E-selectin- but not P-selectin-expressing CHO cells. Sambucus nigra lectin, specific for the sialyl-2,6 beta Gal/GalNAc linkage, inhibited P-selectin but not E-selectin binding to HL60 cells. Although sialic acid and Le(x) are components of the P-selectin ligand and the E-selectin ligand, these results indicate that the ligands are related, having overlapping specificities, but are structurally distinct. A protein component containing sialyl Le(x) in proximity to sialyl-2,6 beta Gal structures on the P-selectin ligand may contribute to its specificity for P-selectin.

摘要

血小板和内皮细胞上的P-选择素以及内皮细胞上的E-选择素是白细胞受体,可识别中性粒细胞和单核细胞上的谱系特异性碳水化合物。这些受体的假定配体含有Le(x)核心和唾液酸。由于其他研究人员已表明E-选择素和P-选择素均与唾液酸化的Le(x)结合,我们评估了E-选择素和P-选择素是否识别白细胞上相同的反受体。研究了HL60细胞与表达P-选择素或E-选择素的中国仓鼠卵巢(CHO)细胞之间的相互作用。为了确定除唾液酸化Le(x)外,P-选择素或E-选择素识别是否还需要蛋白质成分,用包括胰凝乳蛋白酶、弹性蛋白酶、蛋白酶Glu-C、无花果蛋白酶、木瓜蛋白酶或嗜热菌蛋白酶在内的蛋白酶消化HL60细胞或中性粒细胞。用这些蛋白酶处理的细胞可结合E-选择素,但不能结合P-选择素。用岩藻糖苷酶或神经氨酸酶处理HL60细胞可显著降低其与表达E-选择素和P-选择素的CHO细胞的结合。衣霉素处理HL60细胞的生长抑制了这些细胞支持P-选择素介导的结合的能力,对E-选择素介导的结合的抑制作用较小。纯化的P-选择素可抑制CHO:P-选择素与HL60细胞的结合,但不能完全抑制CHO:E-选择素与HL60细胞的结合。然而,纯化的可溶性E-选择素可等效且完全地抑制CHO:P-选择素和CHO:E-选择素与HL60细胞的结合。COS细胞无法与E-选择素或P-选择素结合,在用α-1,3-岩藻糖基转移酶或α-1,3/1,4-岩藻糖基转移酶转染后可结合E-选择素但不能结合P-选择素。同样,表达唾液酸化Le(x)的LEC 11细胞可结合表达E-选择素但不结合表达P-选择素的CHO细胞。黑接骨木凝集素对唾液酸化-2,6βGal/GalNAc连接具有特异性,可抑制P-选择素与HL60细胞的结合,但不能抑制E-选择素与HL60细胞的结合。尽管唾液酸和Le(x)是P-选择素配体和E-选择素配体的成分,但这些结果表明这些配体相关,具有重叠的特异性,但在结构上是不同的。P-选择素配体上靠近唾液酸化-2,6βGal结构的含有唾液酸化Le(x)的蛋白质成分可能有助于其对P-选择素的特异性。

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