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Effect of Variation in hemorheology between human and animal blood on the binding efficacy of vascular-targeted carriers

机译:人和动物血液血液流变学变化对血管靶向载体结合功效的影响

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摘要

Animal models are extensively used to evaluate the in vivo functionality of novel drug delivery systems (DDS). However, many variations likely exist in vivo between the animals and human physiological environment that significantly alter results obtained with animal models relative to human system. To date, it is not clear if the variation in hemorheology and hemodynamics between common animal and human models affect the functionality of DDS. This study investigates the role of hemorheology of humans and various animal models in dictating the binding efficiency of model vascular-targeted carriers (VTCs) to the wall in physiological blood flows. Specifically, the adhesion of sLeA-coated nano- and micro-spheres to inflamed endothelial cells monolayers were conducted via a parallel plate flow chamber assay with steady and disturbed red blood cells (RBCs)-in-buffer and whole blood flows of common animal models. Our results suggest that the ratio of carrier size to RBC size dictate particle binding in blood flow. Additionally, the presence of white blood cells affects the trend of particle adhesion depending on the animal species. Overall, this work sheds light on some deviation in VTC vascular wall interaction results obtained with in vivo animal experimentation from expected outcome and efficiency in vivo in human.
机译:动物模型被广泛用于评估新型药物递送系统(DDS)的体内功能。但是,在动物和人类生理环境之间的体内可能存在许多变异,这大大改变了相对于人类系统,用动物模型获得的结果。迄今为止,尚不清楚常见动物模型和人体模型之间血液流变学和血液动力学的变化是否会影响DDS的功能。这项研究调查了人类血液流变学和各种动物模型在决定模型血管靶向载体(VTC)与生理血流壁之间的结合效率中的作用。具体而言,通过平行板流室测定法在稳定且受干扰的红细胞(RBC)缓冲液中进行sLe A 涂层的纳米球和微球对发炎的内皮细胞单层的粘附和普通动物模型的全血流量。我们的结果表明,载体大小与RBC大小之比决定了血流中的颗粒结合。另外,取决于动物种类,白细胞的存在影响颗粒粘附的趋势。总的来说,这项工作揭示了在体内动物实验中获得的VTC血管壁相互作用结果与人体内预期结果和效率之间的某些偏差。

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