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血管靶向微球在人体微血管微流模型中血流的边缘倾向。

Margination propensity of vascular-targeted spheres from blood flow in a microfluidic model of human microvessels.

机构信息

Department of Biomedical Engineering, University of Michigan, Ann Arbor, Michigan 48109-2136, USA.

出版信息

Langmuir. 2013 Feb 26;29(8):2530-5. doi: 10.1021/la304746p. Epub 2013 Feb 8.

Abstract

Many variants of vascular-targeted carriers (VTCs) have been investigated for therapeutic intervention in several human diseases. However, in order to optimize the functionality of VTC in vivo, carriers' physical properties, such as size and shape, are important considerations for a VTC design that evades the reticuloendothelial system (RES) and successfully interacts with the targeted vessel wall. Nonetheless, little evidence has been presented on the role of size in VTC's interactions with the vascular wall, particularly in the microcirculation. Thus, in this work, we explore how particle size, along with hemodynamics (blood shear rate and vessel size) and hemorheology (blood hematocrit) affect the capacity for spheres to marginate (localize and adhere) to inflamed endothelium in a microfluidic model of human microvessels. Microspheres, particularly the 2 μm spheres, were found to show disproportionately higher margination than nanospheres in all hemodynamic conditions evaluated due to the poor ability of the latter to localize to the wall region from midstream. This work represents the first evidence that nanospheres may not exhibit "near wall excess" in microvessels, e.g., arterioles and venules, and therefore may not be suitable for imaging and drug delivery applications in cancer and other diseases affecting microvessels.

摘要

许多血管靶向载体 (VTC) 的变体已被用于治疗多种人类疾病。然而,为了优化 VTC 在体内的功能,载体的物理性质,如大小和形状,是设计 VTC 时需要考虑的重要因素,以避免网状内皮系统 (RES) 并成功与靶向血管壁相互作用。然而,很少有证据表明大小在 VTC 与血管壁相互作用中的作用,特别是在微循环中。因此,在这项工作中,我们探讨了粒径以及血液动力学(血液剪切率和血管大小)和血液流变学(血液血细胞比容)如何影响球体在人类微血管的微流控模型中定位于(局部化和粘附)发炎的内皮的能力。由于后者难以从中游定位到壁区,因此微球,特别是 2μm 微球,在评估的所有血流动力学条件下都表现出不成比例的更高定位于比纳米球,这是由于后者难以从中游定位到壁区。这项工作首次证明纳米球在微脉管中(例如,小动脉和小静脉)可能不会表现出“近壁过剩”,因此可能不适合用于癌症和其他影响微脉管的疾病的成像和药物输送应用。

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