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小于 100nm 的聚合物胶束在通透性差的肿瘤中的积累取决于粒径大小。

Accumulation of sub-100 nm polymeric micelles in poorly permeable tumours depends on size.

机构信息

Department of Bioengineering, Graduate School of Engineering, The University of Tokyo, Hongo, Bunkyo-ku, Japan.

出版信息

Nat Nanotechnol. 2011 Oct 23;6(12):815-23. doi: 10.1038/nnano.2011.166.

Abstract

A major goal in cancer research is to develop carriers that can deliver drugs effectively and without side effects. Liposomal and particulate carriers with diameters of ∼100 nm have been widely used to improve the distribution and tumour accumulation of cancer drugs, but so far they have only been effective for treating highly permeable tumours. Here, we compare the accumulation and effectiveness of different sizes of long-circulating, drug-loaded polymeric micelles (with diameters of 30, 50, 70 and 100 nm) in both highly and poorly permeable tumours. All the polymer micelles penetrated highly permeable tumours in mice, but only the 30 nm micelles could penetrate poorly permeable pancreatic tumours to achieve an antitumour effect. We also showed that the penetration and efficacy of the larger micelles could be enhanced by using a transforming growth factor-β inhibitor to increase the permeability of the tumours.

摘要

癌症研究的一个主要目标是开发能够有效且无副作用地输送药物的载体。直径约为 100nm 的脂质体和颗粒载体已被广泛用于改善癌症药物的分布和肿瘤积累,但到目前为止,它们仅对治疗高通透性肿瘤有效。在这里,我们比较了不同大小的长循环、载药聚合物胶束(直径为 30nm、50nm、70nm 和 100nm)在高渗透性和低渗透性肿瘤中的积累和效果。所有聚合物胶束都能穿透高通透性肿瘤,但只有 30nm 的胶束能够穿透低通透性的胰腺肿瘤,从而发挥抗肿瘤作用。我们还表明,通过使用转化生长因子-β抑制剂来增加肿瘤的通透性,可以增强较大胶束的穿透性和功效。

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