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Normalization of tumour blood vessels improves the delivery of nanomedicines in a size-dependent manner

机译:肿瘤血管的正常化以尺寸依赖性方式改善纳米药物的递送

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摘要

The blood vessels of cancerous tumours are leaky and poorly organized. This can increase the interstitial fluid pressure inside tumours and reduce blood supply to them, which impairs drug delivery. Anti-angiogenic therapies—which ‘normalize’ the abnormal blood vessels in tumours by making them less leaky—have been shown to improve the delivery and effectiveness of chemotherapeutics with low molecular weights, but it remains unclear whether normalizing tumour vessels can improve the delivery of nanomedicines. Here, we show that repairing the abnormal vessels in mammary tumours, by blocking vascular endothelial growth factor receptor-2, improves the delivery of smaller nanoparticles (diameter, 12 nm) while hindering the delivery of larger nanoparticles (diameter, 125 nm). Using a mathematical model, we show that reducing the sizes of pores in the walls of vessels through normalization decreases the interstitial fluid pressure in tumours, thus allowing small nanoparticles to enter them more rapidly. However, increased steric and hydrodynamic hindrances, also associated with smaller pores, make it more difficult for large nanoparticles to enter tumours. Our results further suggest that smaller (~12 nm) nanomedicines are ideal for cancer therapy due to their superior tumour penetration.
机译:癌性肿瘤的血管渗漏且组织不良。这会增加肿瘤内部的组织液压力并减少血液供应,从而削弱药物的输送。抗血管生成疗法(通过减少渗漏使肿瘤中的异常血管“正常化”)已被证明可以改善低分子量化疗药物的递送和有效性,但尚不清楚使肿瘤血管正常化是否可以改善肿瘤的递送。纳米药物。在这里,我们表明,通过阻断血管内皮生长因子受体2来修复乳腺肿瘤中的异常血管,可改善较小纳米颗粒(直径12 nm)的输送,同时又会阻碍较大纳米颗粒(直径125 nm)的输送。使用数学模型,我们表明通过归一化减小血管壁中的孔的大小会降低肿瘤中的组织液压力,从而使小的纳米颗粒能够更快地进入它们。然而,增加的空间和流体动力障碍,也与较小的孔有关,使得较大的纳米颗粒更难以进入肿瘤。我们的结果进一步表明,较小的(〜12 nm)纳米药物由于其优异的肿瘤渗透性而非常适合癌症治疗。

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