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凝血酶对单核细胞与人内皮细胞单层结合的刺激作用。

Stimulation of mononuclear cell binding to human endothelial cell monolayers by thrombin.

作者信息

Saegusa Y, Cavender D, Ziff M

机构信息

Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas 75235-9030.

出版信息

J Immunol. 1988 Dec 15;141(12):4140-5.

PMID:3058799
Abstract

The common occurrence of fibrin deposits in chronic inflammatory lesions suggests a possible role for thrombin in the mobilization of mononuclear cell infiltrates. For this reason, the effect of thrombin on the binding of mononuclear cells to endothelial cells (EC) was investigated. Incubation of confluent monolayers of human umbilical vein endothelial cells with thrombin markedly enhanced EC adhesiveness for both T lymphocytes and U937 cells (a monocyte-like cell line) in a time- and dose-dependent fashion. This effect was EC specific: 1) treatment of the T cells or the U937 cells with thrombin did not stimulate their adherence to EC, and 2) treatment of human foreskin fibroblasts with thrombin did not stimulate their inherently low adhesiveness for T cells. Fixation of EC monolayers with paraformaldehyde after pre-incubation with thrombin did not affect the increased adhesiveness for T cells. mAb against the LFA-1 antigen (mAb 60.3 (anti-CD18) or mAb TS1/22 (anti-CD11a), which inhibit the binding of T cells to unstimulated EC, failed to block the increased adhesion induced by thrombin, indicating that the increased binding induced by thrombin is similar to that induced by IL-1 and TNF, which showed similar resistance. These results suggest that thrombin may have a role in the extravascular emigration of mononuclear cells from post-capillary venules by virtue of its ability to stimulate the adhesiveness of EC for both lymphocytes and monocytes.

摘要

纤维蛋白沉积物在慢性炎症病变中普遍存在,这表明凝血酶在单核细胞浸润的动员过程中可能发挥作用。基于此,研究了凝血酶对单核细胞与内皮细胞(EC)结合的影响。用人脐静脉内皮细胞的汇合单层与凝血酶孵育,以时间和剂量依赖性方式显著增强了EC对T淋巴细胞和U937细胞(一种单核细胞样细胞系)的粘附性。这种作用具有EC特异性:1)用凝血酶处理T细胞或U937细胞不会刺激它们对EC的粘附,2)用凝血酶处理人包皮成纤维细胞不会刺激它们对T细胞固有的低粘附性。在用凝血酶预孵育后用多聚甲醛固定EC单层,不会影响对T细胞增加的粘附性。针对LFA-1抗原的单克隆抗体(抑制T细胞与未刺激的EC结合的mAb 60.3(抗CD18)或mAb TS1/22(抗CD11a))未能阻断凝血酶诱导的粘附增加,表明凝血酶诱导的结合增加与IL-1和TNF诱导的相似,后者表现出类似的抗性。这些结果表明,凝血酶可能通过其刺激EC对淋巴细胞和单核细胞的粘附性的能力,在单核细胞从毛细血管后微静脉的血管外迁移中发挥作用。

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