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载药沸石咪唑酯骨架的水溶液可控合成及其在体内癌症诊疗中的尺寸效应。

Size-Controlled Synthesis of Drug-Loaded Zeolitic Imidazolate Framework in Aqueous Solution and Size Effect on Their Cancer Theranostics in Vivo.

出版信息

ACS Appl Mater Interfaces. 2018 Dec 12;10(49):42165-42174. doi: 10.1021/acsami.8b17660. Epub 2018 Nov 29.

Abstract

Recently, metal-organic frameworks (MOFs) or coordination polymers have shown great potential for drug delivery, yet little has been done to study how particle size affects their tumor targeting and other in vivo features. This plight is probably due to two challenges: (1) the lack of a biocompatible method to precisely control the size of drug-loaded MOFs and (2) the lack of a robust and facile radiolabeling technique to trace particles in vivo. Here, we report a one-pot, rapid, and completely aqueous approach that can precisely tune the size of drug-loaded MOF at room temperature. A chelator-free Cu-labeled method was developed by taking the advantage of this rapid and aqueous synthesis. Cancer cells were found to take drug-loaded MOFs in a size-dependent manner. The in vivo biodistribution of drug-loaded MOF was analyzed with positron emission tomography imaging, which, as far as we know, was used for the first time to quantitatively evaluate MOF in living animals, unveiling that 60 nm MOF showed longer blood circulation and over 50% higher tumor accumulation than 130 nm MOF. Altogether, this size-controlled method helps to find the optimal size of MOF as a drug carrier and opens new possibilities to construct multifunctional delivery systems for cancer theranostics.

摘要

最近,金属-有机骨架(MOFs)或配位聚合物在药物传递方面显示出巨大的潜力,但对于颗粒大小如何影响其肿瘤靶向和其他体内特性的研究还很少。这种困境可能是由于两个挑战造成的:(1)缺乏一种生物相容性的方法来精确控制载药 MOF 的大小,(2)缺乏一种强大而简单的放射性标记技术来追踪体内的颗粒。在这里,我们报告了一种在室温下可以精确调节载药 MOF 尺寸的一锅法、快速和完全水性的方法。利用这种快速和水性的合成方法,开发了一种无螯合剂的 Cu 标记方法。发现癌细胞以尺寸依赖的方式摄取载药 MOF。通过正电子发射断层扫描成像分析了载药 MOF 的体内生物分布,据我们所知,这是首次用于在活体动物中定量评估 MOF,结果表明 60nm MOF 的血液循环时间比 130nm MOF 长 50%以上,肿瘤积累量也高 50%以上。总的来说,这种尺寸控制方法有助于找到作为药物载体的 MOF 的最佳尺寸,并为构建癌症治疗的多功能递药系统开辟了新的可能性。

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