首页> 外文期刊>Journal of thrombosis and thrombolysis >A novel dynamic layer-by-layer assembled nano-scale biointerface: Functionality tests with platelet adhesion and aggregate morphology influenced by adenosine diphosphate
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A novel dynamic layer-by-layer assembled nano-scale biointerface: Functionality tests with platelet adhesion and aggregate morphology influenced by adenosine diphosphate

机译:一种新型的动态逐层组装的纳米级生物界面:功能测试,受血小板粘附和聚集形态的影响,磷酸腺苷二磷酸

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摘要

An improved biointerface was developed, dynamic layer-by-layer self-assembly surface (d-LbL), and utilized as a biologically-active substrate for platelet adhesion and aggregation. Possible clinical applications for this research include improved anti-coagulation surfaces. This work demonstrated the functionality of d-LbL biointerfaces in the presence of platelet-rich-plasma (PRP) with the addition of 20 μM adenosine diphosphate (ADP), a thrombus activator. The surface morphology of the experimental control, plain PRP, was compared to PRP containing additional ADP (PRP + ADP) and resulted in an expected increase of platelet adhesions along the fibrinogen d-LbL substrate. The d-LbL process was used to coat glass slides with fibrinogen, Poly (sodium 4-styrene-sulfonate), and Poly (diallydimethlyammonium chloride). Slides were exposed to PRP under flow and static conditions with and without 20 μM of ADP. Fluorescence microscopy (FM), phase contrast microscopy (PCM), atomic force microscopy (AFM), and field emission-scanning electron microscopy (FE-SEM) were used to evaluate platelet adhesions under the influence of varied shear conditions. PCM images illustrated differences between the standard LbL and d-LbL substrates. FM images provided percent surface coverage values. For high-shear conditions, percent surface coverage values increased when using ADP whereas plain PRP exposure displayed no significant increase. AFM scans also displayed higher mean peak height values and unique surface characteristics for PRP + ADP as opposed to plain PRP. FE-SEM images revealed platelet adhesions along the biointerface and unique characteristics of the d-LbL surface. In conclusion, PRP + ADP was more effective at increasing platelet aggregation, especially under high shear conditions, providing further validation of the improved biointerface.
机译:开发了一种改进的生物界面,动态的逐层自组装表面(d-LbL),并用作血小板粘附和聚集的生物活性基质。该研究可能的临床应用包括改进的抗凝表面。这项工作证明了在富血小板血浆(PRP)的存在下添加20μM血栓激活剂腺苷二磷酸(ADP)时d-LbL生物界面的功能。将实验对照的普通PRP的表面形态与包含其他ADP的PRP(PRP + ADP)进行了比较,结果表明沿纤维蛋白原d-LbL底物的血小板粘附性有望增加。 d-LbL工艺用于在玻片上涂上纤维蛋白原,聚(4-苯乙烯磺酸钠)和聚(二烯丙基二甲基氯化铵)。在有和没有20μMADP的流动和静态条件下,将玻片暴露于PRP。荧光显微镜(FM),相衬显微镜(PCM),原子力显微镜(AFM)和场发射扫描电子显微镜(FE-SEM)用于评估在不同剪切条件下的血小板粘附。 PCM图像说明了标准LbL和d-LbL基板之间的差异。 FM图像提供了百分比的表面覆盖率值。对于高剪切条件,当使用ADP时,表面覆盖率百分比增加,而普通PRP暴露则无明显增加。与普通PRP相比,AFM扫描还显示出较高的平均峰高值和PRP + ADP的独特表面特性。 FE-SEM图像显示了沿生物界面的血小板粘附以及d-LbL表面的独特特征。总之,PRP + ADP在增加血小板聚集方面更有效,尤其是在高剪切条件下,从而进一步验证了改善的生物界面。

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