Komissarov Andrey A, Mazar Andrew P, Koenig Kathy, Kurdowska Anna K, Idell Steven
Texas Lung Injury Institute of The University of Texas Health Science Center at Tyler, Tyler, Texas 75708, USA.
Am J Physiol Lung Cell Mol Physiol. 2009 Oct;297(4):L568-77. doi: 10.1152/ajplung.00066.2009. Epub 2009 Aug 7.
The proenzyme single-chain urokinase plasminogen activator (scuPA) more effectively resolved intrapleural loculations in rabbits with tetracycline (TCN)-induced loculation than a range of clinical doses of two-chain uPA (Abbokinase) and demonstrated a trend toward greater efficacy than single-chain tPA (Activase) (Idell S et al., Exp Lung Res 33: 419, 2007.). scuPA more slowly generates durable intrapleural fibrinolytic activity than Abbokinase or Activase, but the interactions of these agents with inhibitors in pleural fluids (PFs) have been poorly understood. PFs from rabbits with TCN-induced pleural injury treated with intrapleural scuPA, its inactive Ser195Ala mutant, Abbokinase, Activase, or vehicle, were analyzed to define the mechanism by which scuPA induces durable fibrinolysis. uPA activity was elevated in PFs of animals treated with scuPA, correlated with the ability to clear pleural loculations, and resisted (70-80%) inhibition by PAI-1. Alpha-macroglobulin (alphaM) but not urokinase receptor complexes immunoprecipitated from PFs of scuPA-treated rabbits retained uPA activity that resists PAI-1 and activates plasminogen. Conversely, little plasminogen activating or enzymatic activity resistant to PAI-1 was detectable in PFs of rabbits treated with Abbokinase or Activase. Consistent with these findings, PAI-1 interacts with scuPA much slower than with Activase or Abbokinase in vitro. An equilibrium between active and inactive scuPA (k(on) = 4.3 h(-1)) limits the rate of its inactivation by PAI-1, favoring formation of complexes with alphaM. These observations define a newly recognized mechanism that promotes durable intrapleural fibrinolysis via formation of alphaM/uPA complexes. These complexes promote uPA-mediated plasminogen activation in scuPA-treated rabbits with TCN-induced pleural injury.
与一系列临床剂量的双链尿激酶型纤溶酶原激活剂(Abbokinase)相比,单链尿激酶型纤溶酶原激活剂(scuPA)在四环素(TCN)诱导形成胸膜粘连的兔体内能更有效地溶解胸膜腔内的粘连,并且显示出比单链组织型纤溶酶原激活剂(Activase)有更高疗效的趋势(Idell S等人,《实验肺研究》33:419,2007年)。scuPA产生持久的胸膜腔内纤溶活性的速度比Abbokinase或Activase慢,但这些药物与胸液(PFs)中抑制剂的相互作用尚不清楚。对用胸膜腔内scuPA、其无活性的Ser195Ala突变体、Abbokinase、Activase或赋形剂处理的TCN诱导胸膜损伤的兔的PFs进行分析,以确定scuPA诱导持久纤溶的机制。接受scuPA治疗的动物的PFs中尿激酶型纤溶酶原激活剂(uPA)活性升高,这与清除胸膜粘连的能力相关,并且能抵抗(70 - 80%)纤溶酶原激活剂抑制物1(PAI - 1)的抑制作用。从接受scuPA治疗的兔的PFs中免疫沉淀的α - 巨球蛋白(αM)而非尿激酶受体复合物保留了抵抗PAI - 1并激活纤溶酶原的uPA活性。相反,在接受Abbokinase或Activase治疗的兔的PFs中,几乎检测不到对PAI - 1有抗性的纤溶酶原激活或酶活性。与这些发现一致,在体外PAI - 1与scuPA的相互作用比与Activase或Abbokinase慢得多。活性和无活性scuPA之间的平衡(k(on) = 4.3 h⁻¹)限制了其被PAI - 1灭活的速率,有利于与αM形成复合物。这些观察结果定义了一种新认识的机制,即通过形成αM/uPA复合物促进持久的胸膜腔内纤溶。这些复合物在接受scuPA治疗的TCN诱导胸膜损伤的兔中促进uPA介导的纤溶酶原激活。