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用于溶栓治疗的尿激酶包被壳聚糖纳米粒:体内制备及药效学

Urokinase-coated chitosan nanoparticles for thrombolytic therapy: preparation and pharmacodynamics in vivo.

作者信息

Jin Hai-jiang, Zhang Hao, Sun Min-li, Zhang Bai-gen, Zhang Ji-wei

机构信息

Department of Vascular Surgery, Ren Ji Hospital, School of Medicine, Shanghai Jiaotong University, No. 145 Shandong Middle Road, Shanghai, China.

出版信息

J Thromb Thrombolysis. 2013 Nov;36(4):458-68. doi: 10.1007/s11239-013-0951-7.

Abstract

Blood reperfusion of affected limbs is the most effective therapy for peripheral vascular thrombotic disease, restoring nutrition and blood flow to threatened tissues. Because it is more cost-effective than other thrombolytics, urokinase (UK) is widely used to treat venous thrombosis in China. However, its use is limited because of the risk of UK-related hemorrhagic complications. UK-coated nanoparticles (NPs) may decrease adverse effects while simultaneously increasing thrombolytic benefits. The aim of this study was to combine the sustained-release properties of NPs with the clinical benefits of catheter-directed thrombolysis (CDT) to create a promising new therapy. NPs were prepared via self-assembled chitosan and tripolyphosphate, introduced into a thrombosis model in New Zealand white rabbits, and the ratio of the residual thrombus cross-sectional area to the vascular cross-sectional area was calculated. The NPs had a drug-bearing efficiency of 14.5 ± 1.3%, an encapsulation efficiency of 94.8 ± 2.1% while the particle size of UK-coated NPs was 236 nm. Transmission electron microscopy results showed that the shape of the NPs were spherical and regular. Whether delivered by intravenation or catheter, UK-coated NPs produced a significant increase in the thrombolytic effect compared with free UK and confirmed the superiority of CDT for improving clot lysis over drug-induced systemic thrombolysis. The intravenous NPs caused an abnormal increase in fibrinogen. In conclusion, a water-soluble UK-WCS-NP suspension with good encapsulation efficiency was easily prepared UK-WCS-NPs were capable of maintaining UK activity, provided sustained-release of UK and exhibited better thrombolytic function than free UK.

摘要

患肢血液再灌注是治疗周围血管血栓性疾病最有效的方法,可恢复对受威胁组织的营养供应和血流。由于尿激酶(UK)比其他溶栓剂更具成本效益,在中国被广泛用于治疗静脉血栓形成。然而,由于UK相关出血并发症的风险,其应用受到限制。载UK纳米颗粒(NPs)可能会减少不良反应,同时增加溶栓益处。本研究的目的是将NPs的缓释特性与导管定向溶栓(CDT)的临床益处相结合,创造一种有前景的新疗法。通过壳聚糖和三聚磷酸钠自组装制备NPs,将其引入新西兰白兔血栓形成模型中,并计算残余血栓横截面积与血管横截面积的比值。NPs的载药效率为14.5±1.3%,包封率为94.8±2.1%,而载UK NPs的粒径为236nm。透射电子显微镜结果显示NPs形状为球形且规则。无论是通过静脉注射还是导管给药,与游离UK相比,载UK NPs均显著提高了溶栓效果,并证实了CDT在改善血栓溶解方面优于药物诱导的全身溶栓。静脉注射NPs导致纤维蛋白原异常增加。总之,易于制备出具有良好包封率的水溶性UK-WCS-NP混悬液,UK-WCS-NPs能够保持UK活性,实现UK的缓释,并且比游离UK表现出更好的溶栓功能。

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