Niedbala M J
Institute of Inflammation and Autoimmunity, Miles Research Center, Miles Inc. West Haven, CT 06516.
Agents Actions Suppl. 1993;42:179-93. doi: 10.1007/978-3-0348-7397-0_15.
The vascular endothelium plays a central role in the regulation of extrinsic fibrinolysis and thus maintains vascular patency through clot dissolution. Plasminogen activation provides an important source of localized proteolytic activity not only during fibrinolysis but also during a variety of other physiological and pathological processes. Numerous studies have indicated that human endothelial cells can directly synthesize and secrete plasminogen activators (PA) and inhibitors of these activators. PAs specifically hydrolyse a single arginine-valine bond in plasminogen, an abundant and widely distributed plasma zymogen, to form the broad spectrum serine protease, plasmin. Tissue type-PA (t-PA) and urokinase type PA (u-PA) forms of PA have been described in endothelial cells, although t-PA production and secretion is elevated most frequently. The tPA form of PA functions predominantly in endothelial cell mediated fibrinolysis, while uPA is involved in tissue remodeling. During inflammatory reactions activated mononuclear phagocytes produce a variety of cytokines which may influence the phenotype of the endothelium through a process termed "endothelial cell activation". Tumor necrosis factor alpha (TNF alpha), a mononuclear cytokine, is a distinct polypeptide of Mr 17,000 and has been implicated as a mediator of gram negative induced sepsis as well as angiogenesis. TNF alpha is known to interact with specific endothelial cell receptors and to alter endothelial coagulant and anticoagulant properties implying that cytokines may be potent modulators of hemostasis. Recent observations have indicated that TNF alpha and lymphotoxin (TNF beta) can promote the expression, synthesis and secretion of urokinase plasminogen activator (uPA) in human endothelial cells. The upregulation of uPA results in an alteration in the fibrinolytic capacity of endothelial cells and allows cells the selective ability to degrade and invade underlying subendothelial extracellular matrix (ECM). Endothelial cells treated with TNF alpha also display, in an in vitro angiogenic assay, the ability to invade Matrigel and reorganize into tube-like structures, unlike control cultures. The effects of TNF alpha on the PA proteolytic system of endothelial cells, the biological significance of this event and potential in vivo consequences will be discussed. In addition, the influence of cytokine regulatory control systems will be described, since it is becoming increasingly clear that cytokines do not act in isolation. The vascular endothelium serves as a widely distributed anatomical interface between the blood and tissue with diverse capabilities, performing distinctive biologic functions at different sites and within specific organs.(ABSTRACT TRUNCATED AT 400 WORDS)
血管内皮在调节外源性纤维蛋白溶解过程中起核心作用,从而通过血栓溶解维持血管通畅。纤溶酶原激活不仅在纤维蛋白溶解过程中,而且在各种其他生理和病理过程中,都提供了局部蛋白水解活性的重要来源。大量研究表明,人内皮细胞可直接合成和分泌纤溶酶原激活剂(PA)及其激活剂的抑制剂。PA特异性水解血浆中丰富且广泛分布的酶原——纤溶酶原中的单个精氨酸 - 缬氨酸键,形成广谱丝氨酸蛋白酶——纤溶酶。在内皮细胞中已发现组织型PA(t - PA)和尿激酶型PA(u - PA)形式的PA,尽管t - PA的产生和分泌最为常见。PA的tPA形式主要在内皮细胞介导的纤维蛋白溶解中起作用,而uPA参与组织重塑。在炎症反应期间,活化的单核吞噬细胞产生多种细胞因子,这些细胞因子可能通过一种称为“内皮细胞活化”的过程影响内皮细胞的表型。肿瘤坏死因子α(TNFα)是一种单核细胞因子,是一种分子量为17,000的独特多肽,被认为是革兰氏阴性菌诱导的败血症以及血管生成的介质。已知TNFα与特定的内皮细胞受体相互作用,并改变内皮细胞的凝血和抗凝特性,这意味着细胞因子可能是止血的有效调节剂。最近的观察表明,TNFα和淋巴毒素(TNFβ)可促进人内皮细胞中尿激酶纤溶酶原激活剂(uPA)的表达、合成和分泌。uPA的上调导致内皮细胞纤溶能力的改变,并使细胞具有降解和侵入下层内皮下细胞外基质(ECM)的选择性能力。用TNFα处理的内皮细胞在体外血管生成试验中也表现出侵入基质胶并重组为管状结构的能力,这与对照培养不同。将讨论TNFα对内皮细胞PA蛋白水解系统的影响、这一事件的生物学意义以及潜在的体内后果。此外,还将描述细胞因子调节控制系统的影响,因为越来越清楚的是细胞因子并非单独起作用。血管内皮是血液与组织之间广泛分布的解剖学界面,具有多种功能,在不同部位和特定器官内执行独特的生物学功能。(摘要截选至400字)
