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首页> 外文期刊>Microcirculation: The official journal of the Microcirculatory Society >Soluble P-selectin antagonist mediates rolling velocity and adhesion of leukocytes in acutely inflamed venules.
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Soluble P-selectin antagonist mediates rolling velocity and adhesion of leukocytes in acutely inflamed venules.

机译:可溶性P-选择素拮抗剂介导急性发炎的小静脉的滚动速度和白细胞粘附。

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OBJECTIVE: Leukocyte rolling is recognized as an important event in facilitating the extravasation of leukocytes from the vascular to the interstitial compartment, and is mediated by the selectin family of cell adhesion molecules. The aim of this study was to evaluate and characterize the rolling behavior of leukocytes in a model of acute inflammation using a novel soluble selectin ligand directed against P-selectin. METHODS: Feline mesenteric postcapillary venules were visualized using intravital microscopy prior to and following exposure to leukotriene C4 (LTC4) in animals pretreated with vehicle (saline) and the P-selectin antagonist rPSGL-Ig. RESULTS: A concentration of 500 pM LTC4 induced a threefold and sixfold elevation in leukocyte rolling flux and adhesion, respectively, compared to baseline values (p < 0.05). Administration of rPSGL-Ig had no effect on LTC4-induced leukocyte rolling flux but significantly attenuated the increase in the fraction of rolling leukocytes (p < 0.05). In addition, rPSGL-Ig inhibited the LTC4-induced reductions in leukocyte rolling velocity (p < 0.001). Finally, LTC4-induced leukocyte adhesion in animals pretreated with rPSGL-Ig was reduced by 60%, compared to vehicle-treated animals (p < 0.05). CONCLUSIONS: LTC4 induces leukocyte rolling and adhesion in feline mesenteric venules in a dose-dependent manner. Administration of rPSGL-Ig inhibits LTC4-induced reductions in leukocyte rolling velocity and attenuates the elevation in the fraction of rolling leukocytes produced by LTC4 stimulation. This suggests that rPSGL-Ig may be used to reduce leukocyte rolling and adhesion, and subsequently attenuate tissue injury during inflammation.
机译:目的:白细胞滚动被认为是促进白细胞从血管向间质渗出的重要事件,并且是由细胞粘附分子的选择素家族介导的。这项研究的目的是使用针对P选择素的新型可溶性选择素配体评估和表征急性炎症模型中白细胞的滚动行为。方法:在用媒介物(盐水)和P-选择素拮抗剂rPSGL-Ig预处理的动物中,暴露于白三烯C4(LTC4)之前和之后,使用活体显微镜对猫肠系膜后毛细血管进行可视化。结果:与基线值相比,浓度为500 pM LTC4引起白细胞滚动通量和粘附力分别升高三倍和六倍(p <0.05)。施用rPSGL-Ig对LTC4诱导的白细胞滚动通量无影响,但显着减弱了滚动白细胞分数的增加(p <0.05)。另外,rPSGL-Ig抑制了LTC4诱导的白细胞滚动速度降低(p <0.001)。最后,与用赋形剂处理的动物相比,用rPSGL-Ig预处理的动物中LTC4诱导的白细胞粘附降低了60%(p <0.05)。结论:LTC4以剂量依赖的方式诱导猫肠系膜小静脉的白细胞滚动和粘附。施用rPSGL-Ig可抑制LTC4诱导的白细胞滚动速度降低,并减弱LTC4刺激产生的滚动白细胞分数的升高。这表明rPSGL-Ig可用于减少白细胞滚动和粘附,并随后减轻炎症期间的组织损伤。

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