首页> 外文期刊>American Journal of Physiology >Selective recruitment of neutrophils and lymphocytes by thrombin: a role for NF-kappaB.
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Selective recruitment of neutrophils and lymphocytes by thrombin: a role for NF-kappaB.

机译:凝血酶选择性募集中性粒细胞和淋巴细胞:NF-κB的作用。

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摘要

With the use of a whole blood laminar flow chamber system, we examined the types of leukocytes, adhesion molecules and the role of nuclear factor-kappaB (NF-kappaB) in thrombin-induced leukocyte recruitment. Primary human umbilical vein endothelial cells (HUVEC) stimulated with thrombin induced a significant increase in P-selectin-dependent neutrophil recruitment. Unexpectedly, brief thrombin stimulation (3 min) of endothelium also induced a significant lymphocyte recruitment 4 h later in addition to neutrophil recruitment. E-selectin antibody reduced neutrophil recruitment by >90%, whereas vascular adhesion molecule-1 (VCAM-1)/alpha4-integrin were primarily responsible for lymphocyte recruitment. To examine whether NF-kappaB contributed to leukocyte recruitment 4 h post thrombin stimulation, we treated HUVEC with the NF-kappaB inhibitor MG-132 for 1 h before thrombin stimulation. MG-132 significantly reduced the number of rolling (77.1%) and adherent (79.9%) leukocytes compared with thrombin stimulation alone. The inhibitor was more effective at preventing lymphocyte than neutrophil recruitment, consistent with its greater effect on VCAM-1 versus E-selectin expression. Tumor necrosis factor-alpha- and MG-132-treated HUVEC displayed no inhibition of leukocyte recruitment despite a decrease in NF-kappaB activation. In summary, thrombin causes predominant neutrophil recruitment via rapid P-selectin expression but also a delayed E-selectin- and VCAM-1-dependent neutrophil and lymphocyte recruitment via de novo protein synthesis. Although NF-kappaB mobilization was essential for thrombin-mediated VCAM-1-dependent recruitment, it only partially contributed to E-selectin-dependent recruitment.
机译:通过使用全血层流腔系统,我们检查了白细胞的类型,粘附分子以及核因子-κB(NF-kappaB)在凝血酶诱导的白细胞募集中的作用。凝血酶刺激的原代人脐静脉内皮细胞(HUVEC)诱导P-选择素依赖性中性粒细胞募集明显增加。出乎意料的是,除了中性粒细胞募集外,短暂的凝血酶刺激(3分钟)内皮还诱导了4小时后显着的淋巴细胞募集。 E-选择素抗体使嗜中性粒细胞的募集减少了90%以上,而血管粘附分子1(VCAM-1)/α4-整联蛋白主要负责淋巴细胞募集。为了检查凝血酶刺激后4小时NF-κB是否有助于白细胞募集,我们在凝血酶刺激前1小时用NF-κB抑制剂MG-132处理HUVEC。与单独的凝血酶刺激相比,MG-132显着减少了滚动白细胞(77.1%)和粘附白细胞(79.9%)的数量。与中性粒细胞募集相比,该抑制剂在预防淋巴细胞方面更有效,这与其对VCAM-1的影响相比对E-选择素的表达更大。尽管NF-κB活化降低,但肿瘤坏死因子-α和MG-132治疗的HUVEC未显示出对白细胞募集的抑制。总之,凝血酶通过快速的P-选择素表达引起主要的嗜中性白细胞募集,但也通过从头蛋白质合成引起延迟的E-选择素和VCAM-1依赖性嗜中性白细胞和淋巴细胞募集。尽管NF-κB动员对于凝血酶介导的VCAM-1依赖性募集至关重要,但它仅部分促成E-选择素依赖性募集。

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