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GlyCAM-1支持白细胞在血流中滚动:淋巴细胞L-选择素滚动的动态稳定性比中性粒细胞更强的证据。

GlyCAM-1 supports leukocyte rolling in flow: evidence for a greater dynamic stability of L-selectin rolling of lymphocytes than of neutrophils.

作者信息

Dwir O, Shimron F, Chen C, Singer M S, Rosen S D, Alon R

机构信息

Department of Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Cell Adhes Commun. 1998;6(4):349-70. doi: 10.3109/15419069809010793.

DOI:10.3109/15419069809010793
PMID:9865468
Abstract

L-selectin plays a major role in leukocyte traffic through lymph node high endothelial venules (HEV). We have investigated the role of GlyCAM-1, a major L-selectin ligand produced by HEV, in mediating leukocyte rolling under in vitro flow conditions. Purified GlyCAM-1 was found to support tethering and rolling in physiological shear flow of both human and murine L-selectin expressing leukocytes at an efficiency comparable to the HEV-derived L-selectin ligands termed peripheral node addressin (PNAd). Major dynamic differences between L-selectin rolling of peripheral blood T lymphocytes and neutrophils expressing similar L-selectin level were observed on GlyCAM-1. Lymphocytes established slower and more shear resistant rolling than neutrophils and could roll on GlyCAM-1 at shear stresses lower than the threshold values required for L-selectin-mediated neutrophil rolling. Notably, high stability of L-selectin rolling of lymphocytes requires intact cellular energy, although initial lymphocyte tethering to L-selectin ligands is energy-independent. By contrast, L-selectin mediated rolling of neutrophils is insensitive to energy depletion. The distinct dynamic behavior and energy-dependence of L-selectin rolling in different leukocytes suggest that L-selectin adhesiveness in shear flow is regulated in a cell-type specific manner. The greater stability of L-selectin rolling of lymphocytes on surface-adsorbed GlyCAM-1 may contribute to their selective recruitment at peripheral lymph nodes.

摘要

L-选择素在白细胞通过淋巴结高内皮微静脉(HEV)的迁移过程中起主要作用。我们研究了由HEV产生的主要L-选择素配体GlyCAM-1在体外流动条件下介导白细胞滚动中的作用。发现纯化的GlyCAM-1能够支持表达人及鼠L-选择素的白细胞在生理剪切流中进行系留和滚动,其效率与称为外周淋巴结地址素(PNAd)的源自HEV的L-选择素配体相当。在GlyCAM-1上观察到表达相似L-选择素水平的外周血T淋巴细胞和中性粒细胞的L-选择素滚动之间存在主要的动态差异。淋巴细胞比中性粒细胞建立的滚动更慢且更具抗剪切性,并且能够在低于L-选择素介导的中性粒细胞滚动所需阈值的剪切应力下在GlyCAM-1上滚动。值得注意的是,淋巴细胞L-选择素滚动的高稳定性需要完整的细胞能量,尽管淋巴细胞最初与L-选择素配体的系留不依赖能量。相比之下,L-选择素介导的中性粒细胞滚动对能量消耗不敏感。不同白细胞中L-选择素滚动的独特动态行为和能量依赖性表明,剪切流中L-选择素的粘附性是以细胞类型特异性方式调节的。淋巴细胞在表面吸附的GlyCAM-1上L-选择素滚动的更高稳定性可能有助于它们在外周淋巴结的选择性募集。

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1
GlyCAM-1 supports leukocyte rolling in flow: evidence for a greater dynamic stability of L-selectin rolling of lymphocytes than of neutrophils.GlyCAM-1支持白细胞在血流中滚动:淋巴细胞L-选择素滚动的动态稳定性比中性粒细胞更强的证据。
Cell Adhes Commun. 1998;6(4):349-70. doi: 10.3109/15419069809010793.
2
Rolling of lymphocytes and neutrophils on peripheral node addressin and subsequent arrest on ICAM-1 in shear flow.淋巴细胞和中性粒细胞在外周淋巴结地址素上滚动,随后在剪切流中黏附于细胞间黏附分子-1。
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Complexity and differential expression of carbohydrate epitopes associated with L-selectin recognition of high endothelial venules.与L-选择素识别高内皮微静脉相关的碳水化合物表位的复杂性和差异表达。
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Threshold levels of fluid shear promote leukocyte adhesion through selectins (CD62L,P,E).流体剪切力的阈值水平通过选择素(CD62L、P、E)促进白细胞黏附。
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Endomucin, a sialomucin expressed in high endothelial venules, supports L-selectin-mediated rolling.内皮粘液素是一种在内皮高柱状小静脉中表达的唾液酸糖蛋白,它支持L-选择素介导的滚动。
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Leukocyte rolling velocities and migration are optimized by cooperative L-selectin and intercellular adhesion molecule-1 functions.白细胞滚动速度和迁移通过L-选择素与细胞间黏附分子-1的协同作用得以优化。
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Sulfation of a high endothelial venule-expressed ligand for L-selectin. Effects on tethering and rolling of lymphocytes.L-选择素的一种高内皮微静脉表达配体的硫酸化。对淋巴细胞锚定和滚动的影响。
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Neutrophil-neutrophil interactions under hydrodynamic shear stress involve L-selectin and PSGL-1. A mechanism that amplifies initial leukocyte accumulation of P-selectin in vitro.流体动力剪切应力下中性粒细胞与中性粒细胞的相互作用涉及L-选择素和P-选择素糖蛋白配体-1。一种在体外放大P-选择素初始白细胞积聚的机制。
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Expression of GlyCAM-1, an endothelial ligand for L-selectin, is affected by afferent lymphatic flow.L-选择素的内皮配体GlyCAM-1的表达受传入淋巴流的影响。
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引用本文的文献

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Avidity enhancement of L-selectin bonds by flow: shear-promoted rotation of leukocytes turn labile bonds into functional tethers.流动增强L-选择素键的亲和力:剪切力促进白细胞旋转将不稳定键转变为功能性连接。
J Cell Biol. 2003 Nov 10;163(3):649-59. doi: 10.1083/jcb.200303134. Epub 2003 Nov 3.
2
L-selectin shedding does not regulate constitutive T cell trafficking but controls the migration pathways of antigen-activated T lymphocytes.L-选择素的脱落并不调节组成性T细胞运输,但可控制抗原激活的T淋巴细胞的迁移途径。
J Exp Med. 2003 Nov 3;198(9):1323-35. doi: 10.1084/jem.20030485.
3
Tumor cell MUC1 and CD43 are glycosylated differently with sialyl-Lewis a and x epitopes and show variable interactions with E-selectin under physiological flow conditions.
肿瘤细胞MUC1和CD43在唾液酸化刘易斯a和x表位上的糖基化方式不同,并且在生理流动条件下与E-选择素表现出不同的相互作用。
Glycoconj J. 2001 Nov-Dec;18(11-12):925-30. doi: 10.1023/a:1022208727512.
4
Cell-free rolling mediated by L-selectin and sialyl Lewis(x) reveals the shear threshold effect.由L-选择素和唾液酸化路易斯x介导的无细胞滚动揭示了剪切阈值效应。
Biophys J. 2000 Nov;79(5):2391-402. doi: 10.1016/S0006-3495(00)76484-8.
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The chemokine SDF-1 stimulates integrin-mediated arrest of CD34(+) cells on vascular endothelium under shear flow.趋化因子SDF-1在剪切流作用下刺激整合素介导的CD34(+)细胞在血管内皮上的黏附。
J Clin Invest. 1999 Nov;104(9):1199-211. doi: 10.1172/JCI7615.
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Endothelial ligands for L-selectin: from lymphocyte recirculation to allograft rejection.L-选择素的内皮配体:从淋巴细胞再循环到同种异体移植排斥反应
Am J Pathol. 1999 Oct;155(4):1013-20. doi: 10.1016/S0002-9440(10)65201-7.
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Sulfation of a high endothelial venule-expressed ligand for L-selectin. Effects on tethering and rolling of lymphocytes.L-选择素的一种高内皮微静脉表达配体的硫酸化。对淋巴细胞锚定和滚动的影响。
J Exp Med. 1999 Oct 4;190(7):935-42. doi: 10.1084/jem.190.7.935.