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Pharmacokinetic analysis reveals limitations and opportunities for nanomedicine targeting of endothelial and extravascular compartments of tumours

机译:药代动力学分析揭示了纳米医生靶向肿瘤内皮和血管外隔室的局限性和机会

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Targeting of nanoparticles to tumours can potentially improve the specificity of imaging and treatments. We have developed a multicompartmental pharmacokinetic model in order to analyse some of the factors that control efficiency of targeting to intravascular (endothelium) and extravascular (tumour cells and stroma) compartments. We make the assumption that transport across tumour endothelium is an important step for subsequent nanoparticle accumulation in the tumour (area-under-the-curve, AUC) regardless of entry route (interendothelial and transendothelial routes) and study this through a multicompartmental simulation. Our model reveals that increasing endothelial targeting efficiency has a much stronger effect on the AUC than increasing extravascular targeting efficiency. Furthermore, our analysis reveals that both extravasation and intratumoral diffusion rates need to be increased in order to significantly increase the AUC of extravascular-targeted nanoparticles. Increasing the nanoparticle circulation half-life increases the AUC independently of extravasation and intratumoral diffusion. Targeting the extravascular compartment leads to a buildup in the first layer surrounding blood vessels at the expense of deeper layers (binding site barrier). This model explains some of the limitations of tumour targeting and provides important guidelines for the design of targeted nanomedicines.
机译:靶向纳米颗粒至肿瘤可以潜在地改善成像和治疗的特异性。我们开发了一种多组体药代动力学模型,以分析一种控制靶向血管内(内皮)和血管外(肿瘤细胞和基质)隔室效率的一些因素。我们假设肿瘤内皮的运输是随后肿瘤中的纳米颗粒积聚(曲线,AUC)的重要步骤,无论进入途径(间隔性和矫直类途径),通过多组分模拟研究。我们的型号表明,增加内皮靶向效率对AUC的影响更强,而不是提高血管外靶向效率。此外,我们的分析表明,需要增加外渗和肿瘤瘤扩散率,以便显着增加血管靶向纳米颗粒的AUC。增加纳米颗粒循环半衰期随着外渗和脑内扩散而增加AUC。靶向血管外隔室以较深层(结合位点屏障)为代价的血管围绕血管的第一层的堆积。该模型解释了肿瘤靶向的一些局限性,并为目标纳米海运素设计提供了重要指导。

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