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纤溶酶原结合减少和激活延迟使γ'-纤维蛋白比γA-纤维蛋白对溶解更具抗性。

Reduced plasminogen binding and delayed activation render γ'-fibrin more resistant to lysis than γA-fibrin.

作者信息

Kim Paul Y, Vu Trang T, Leslie Beverly A, Stafford Alan R, Fredenburgh James C, Weitz Jeffrey I

机构信息

From the Departments of Medicine, the Thrombosis and Atherosclerosis Research Institute, Hamilton, Ontario L8L 2X2, Canada.

the Thrombosis and Atherosclerosis Research Institute, Hamilton, Ontario L8L 2X2, Canada Biomedical Sciences, and.

出版信息

J Biol Chem. 2014 Oct 3;289(40):27494-503. doi: 10.1074/jbc.M114.588640. Epub 2014 Aug 15.

Abstract

Fibrin (Fn) clots formed from γ'-fibrinogen (γ'-Fg), a variant with an elongated γ-chain, are resistant to lysis when compared with clots formed from the predominant γA-Fg, a finding previously attributed to differences in clot structure due to delayed thrombin-mediated fibrinopeptide (FP) B release or impaired cross-linking by factor XIIIa. We investigated whether slower lysis of γ'-Fn reflects delayed plasminogen (Pg) binding and/or activation by tissue plasminogen activator (tPA), reduced plasmin-mediated proteolysis of γ'-Fn, and/or altered cross-linking. Clots formed from γ'-Fg lysed more slowly than those formed from γA-Fg when lysis was initiated with tPA/Pg when FPA and FPB were both released, but not when lysis was initiated with plasmin, or when only FPA was released. Pg bound to γ'-Fn with an association rate constant 22% lower than that to γA-Fn, and the lag time for initiation of Pg activation by tPA was longer with γ'-Fn than with γA-Fn. Once initiated, however, Pg activation kinetics were similar. Factor XIIIa had similar effects on clots formed from both Fg isoforms. Therefore, slower lysis of γ'-Fn clots reflects delayed FPB release, which results in delayed binding and activation of Pg. When clots were formed from Fg mixtures containing more than 20% γ'-Fg, the upper limit of the normal level, the delay in lysis was magnified. These data suggest that circulating levels of γ'-Fg modulate the susceptibility of clots to lysis by slowing Pg activation by tPA and provide another example of the intimate connections between coagulation and fibrinolysis.

摘要

由γ'-纤维蛋白原(γ'-Fg,一种具有延长γ链的变体)形成的纤维蛋白(Fn)凝块与由主要的γA-Fg形成的凝块相比,对溶解具有抗性,这一发现先前归因于凝血酶介导的纤维蛋白肽(FP)B释放延迟或因子XIIIa交联受损导致的凝块结构差异。我们研究了γ'-Fn溶解较慢是否反映纤溶酶原(Pg)结合延迟和/或组织纤溶酶原激活剂(tPA)激活延迟、γ'-Fn的纤溶酶介导的蛋白水解减少和/或交联改变。当FPA和FPB均释放时,用tPA/Pg启动溶解时,由γ'-Fg形成的凝块比由γA-Fg形成的凝块溶解得更慢,但用纤溶酶启动溶解时,或仅释放FPA时则不然。Pg与γ'-Fn结合的缔合速率常数比与γA-Fn结合的低22%,并且tPA启动Pg激活的延迟时间γ'-Fn比γA-Fn更长。然而,一旦启动,Pg激活动力学是相似的。因子XIIIa对两种Fg同工型形成的凝块具有相似的作用。因此,γ'-Fn凝块溶解较慢反映了FPB释放延迟,这导致Pg结合和激活延迟。当由含有超过20%γ'-Fg(正常水平上限)的Fg混合物形成凝块时,溶解延迟会放大。这些数据表明,γ'-Fg的循环水平通过减缓tPA对Pg的激活来调节凝块对溶解的敏感性,并提供了凝血和纤溶之间密切联系的另一个例子。

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