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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。

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.

作者信息

Walcheck B, Moore K L, McEver R P, Kishimoto T K

机构信息

Department of Immunology, Boehringer Ingelheim Pharmaceuticals, Inc., Ridgefield, Connecticut 06877, USA.

出版信息

J Clin Invest. 1996 Sep 1;98(5):1081-7. doi: 10.1172/JCI118888.

DOI:10.1172/JCI118888
PMID:8787668
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC507527/
Abstract

Leukocytes attach to and roll on inflamed endothelium and on leukocyte monolayers that form on the endothelial cells. Leukocyte-leukocyte interactions occurring under hydrodynamic shear stress are mediated by binding of L-selectin to unknown sialomucin-like glycoproteins. We show that purified neutrophil PSGL-1, a sialomucin glycoprotein that serves as a ligand for both P- and E-selectin, can also support the attachment and rolling of free flowing neutrophils in vitro. Neutrophil rolling on PSGL-1 was abolished by the anti-L-selectin mAb DREG200 and by the anti-PSGL-1 mAb PL1, indicating that L-selectin can interact directly with PSGL-1. Neutrophil rolling on neutrophil monolayers was also blocked by PL1 (60 +/- 9% SEM inhibition); however, DREG200 blocked more efficiently (93 +/- 7% SEM inhibition), suggesting that other L-selectin ligands may exist on the neutrophil surface. These studies demonstrate that PSGL-1 on the neutrophil surface is a major functional ligand for L-selectin. The avidity of this L-selectin-dependent adhesion event was sufficient to allow individual neutrophils rolling on P-selectin to capture free flowing neutrophils, which progressed to form linear strings and discrete foci of rolling neutrophils. Neutrophil accumulation on P-selectin accelerated with time as a result of neutrophil-assisted capture of free flowing neutrophils. When neutrophil-neutrophil interactions were blocked by DREG200, neutrophils accumulated on P-selectin in a random pattern and at a uniform rate. Thus, leukocyte-assisted capture of flowing leukocytes may play an important role in amplifying the rate of initial leukocyte recruitment at sites of inflammation.

摘要

白细胞可附着于炎症部位的内皮细胞并在其上滚动,也可在由内皮细胞形成的白细胞单层上滚动。在流体动力剪切应力作用下发生的白细胞-白细胞相互作用是由L-选择素与未知的唾液酸黏蛋白样糖蛋白结合介导的。我们发现,纯化的中性粒细胞PSGL-1,一种作为P-选择素和E-选择素配体的唾液酸黏蛋白糖蛋白,在体外也能支持自由流动的中性粒细胞的附着和滚动。抗L-选择素单克隆抗体DREG200和抗PSGL-1单克隆抗体PL1可消除中性粒细胞在PSGL-1上的滚动,这表明L-选择素可直接与PSGL-1相互作用。抗PSGL-1单克隆抗体PL1也可阻断中性粒细胞在中性粒细胞单层上的滚动(60±9%,标准误抑制率);然而,DREG200的阻断效果更显著(93±7%,标准误抑制率),这表明中性粒细胞表面可能存在其他L-选择素配体。这些研究表明,中性粒细胞表面的PSGL-1是L-选择素的主要功能配体。这种依赖L-选择素的黏附事件的亲和力足以使单个在P-选择素上滚动的中性粒细胞捕获自由流动的中性粒细胞,进而形成线性串珠和离散的滚动中性粒细胞聚集灶。由于中性粒细胞对自由流动中性粒细胞的辅助捕获,中性粒细胞在P-选择素上的聚集随时间加速。当用DREG200阻断中性粒细胞-中性粒细胞相互作用时,中性粒细胞以随机模式和均匀速率在P-选择素上聚集。因此,白细胞对流动白细胞的辅助捕获可能在炎症部位放大初始白细胞募集速率中起重要作用。

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