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硫酸皮肤素介导的纤维蛋白网络结构的改变。

Alterations of fibrin network structure mediated by dermatan sulfate.

机构信息

Departamento de Química Biológica, Facultad de Ciencias Exactas y Naturales, Universidad de Buenos Aires, Pabellón II, piso 4°, Ciudad Universitaria, C1428EHA Buenos Aires, Argentina.

出版信息

J Thromb Thrombolysis. 2013 Feb;35(2):257-63. doi: 10.1007/s11239-012-0804-9.

Abstract

Dermatan sulfate (DS) is well-known for its anticoagulant activity through binding to heparin cofactor II (HCII) to enhance thrombin inhibition. It has also been reported that DS has a profibrinolytic effect. We have evaluated the effects of DS solutions (4-20 μg/mL) on the formation (by kinetic studies), structure (by electron microscopy and compaction assays) and lysis (with urokinase-type plasminogen activator) of plasma fibrin networks. The results showed that DS significantly prolonged the lag phase and decreased the fibrin formation rate and the optical density of the final networks versus control, in a concentration dependent way. DS-associated networks presented a minor network percentage compared with control, composed of lower number of fibers per field, which resulted significantly thinner and longer. Moreover, DS rendered gels more sensible to rupture by centrifugal force and more susceptible to lysis. When fibrin formation kinetic assays were performed with purified fibrinogen instead of plasma, in the absence of HCII, the optical density of final DS-associated networks was statistically lower than control. Therefore, a direct effect of DS on the thickness of fibers was observed. Since in all in vitro assays low DS concentrations were used, it could be postulated that the fibrin features described above are plausible to be found in in vivo thrombi and therefore, DS would contribute to the formation of less thrombogenic clots.

摘要

硫酸皮肤素(DS)通过与肝素辅因子 II(HCII)结合来增强凝血酶抑制作用而广为人知。据报道,DS 还具有抗纤维蛋白溶解作用。我们评估了 DS 溶液(4-20μg/mL)对血浆纤维蛋白网络形成(通过动力学研究)、结构(通过电子显微镜和压缩测定)和裂解(用尿激酶型纤溶酶原激活物)的影响。结果表明,DS 以浓度依赖的方式显著延长了迟滞期,并降低了纤维蛋白形成速率和最终网络的光密度,与对照相比。与对照相比,DS 相关网络的网络百分比较小,每个视野的纤维数量较少,结果明显更细更长。此外,DS 使凝胶更容易因离心力而破裂,并更容易溶解。当用纯化的纤维蛋白原而不是血浆代替纤维蛋白原进行纤维蛋白形成动力学测定,并且不存在 HCII 时,DS 相关网络的最终光密度比对照明显更低。因此,观察到 DS 对纤维厚度有直接影响。由于在所有体外测定中均使用低浓度的 DS,因此可以假设上述纤维蛋白特征可能在体内血栓中发现,因此 DS 将有助于形成血栓形成性较低的血栓。

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