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红细胞结合型与游离型纤溶酶催化纤维蛋白凝块溶解的空间动力学。

The spatial dynamics of fibrin clot dissolution catalyzed by erythrocyte-bound vs. free fibrinolytics.

机构信息

Department of Cell & Developmental Biology, University of Pennsylvania School of Medicine, Philadelphia, PA 19104-6058, USA.

出版信息

J Thromb Haemost. 2010 May;8(5):1066-74. doi: 10.1111/j.1538-7836.2010.03802.x. Epub 2010 Feb 9.

Abstract

SUMMARY BACKGROUND

Coupling fibrinolytic plasminogen activators to red blood cells (RBCs) has been proposed as an effective, yet safe method of thromboprophylaxis, because of increased circulation lifetime and reduced propensity to induce hemorrhage by selectivity for nascent thrombi rather than pre-formed hemostatic clots.

OBJECTIVES AND METHODS

We used confocal microscopy of fluorescently labeled fibrin and erythrocytes in plasma-derived clots to study the spatial dynamics of lysis catalyzed by RBC-coupled vs. free plasminogen activators (RBC-PA vs. PA).

RESULTS

Clot lysis catalyzed by free PA progressed gradually and uniformly. In contrast, distinct holes formed surrounding RBC-PA while the rest of the clot remained intact until these holes enlarged sufficiently to merge, causing sudden clot dissolution. Compared with naïve RBCs within clots lysed by free PA, RBC-PA moved faster inside the fibrin network prior to clot dissolution, providing a potential mechanism for spatial propagation of RBC-PA induced lysis. We also showed the focal nature of fibrinolysis by RBC-PA as dense loading of PA onto RBCs initiates more efficient lysis than equal amounts of PA spread sparsely over more RBCs. In an in vitro model of clots exposed to buffer flow, incorporated RBC-PA increased permeability and formed channels eventually triggering clot dissolution, whereas clots containing free PA remained intact.

CONCLUSIONS

Clot lysis by RBC-PA begins focally, has a longer lag phase when measured by residual mass than homogeneous lysis by PA, is propagated by RBC-PA motility and provides more effective clot reperfusion than free PA, making RBC-PA attractive for short-term thromboprophylaxis.

摘要

摘要背景

将纤维蛋白溶解酶原激活剂与红细胞(RBC)偶联已被提议作为一种有效的、安全的抗血栓形成方法,因为与选择性针对新生血栓而不是预先形成的止血血栓相比,其循环寿命增加,并且减少了诱导出血的倾向。

目的和方法

我们使用荧光标记的纤维蛋白和血浆来源的凝块中的红细胞的共聚焦显微镜,研究 RBC 偶联与游离纤溶酶原激活剂(RBC-PA 与 PA)催化的纤溶的空间动力学。

结果

游离 PA 催化的血凝块溶解逐渐且均匀地进行。相比之下,在剩余的凝块保持完整的情况下,RBC-PA 周围会形成明显的孔,直到这些孔扩大到足以合并,导致血凝块突然溶解。与在游离 PA 溶解的凝块中溶解的幼稚 RBC 相比,在凝块溶解之前,RBC-PA 在纤维蛋白网络内移动更快,为 RBC-PA 诱导的纤溶的空间传播提供了潜在的机制。我们还展示了 RBC-PA 诱导的纤维蛋白溶解的聚焦性质,因为将 PA 密集加载到 RBC 上比将等量的 PA 稀疏地分散在更多的 RBC 上更有效地引发溶解。在暴露于缓冲液流的体外凝块模型中,掺入的 RBC-PA 增加了通透性并形成了通道,最终触发了凝块溶解,而含有游离 PA 的凝块保持完整。

结论

与 PA 均匀溶解相比,RBC-PA 溶解开始时具有更明显的焦点,残余质量测量的潜伏期更长,由 RBC-PA 运动传播,并提供比游离 PA 更有效的血凝块再灌注,这使得 RBC-PA 成为短期抗血栓形成的有吸引力的方法。

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