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首页> 外文期刊>ACS nano >The Role of Micelle Size in Tumor Accumulation, Penetration, and Treatment
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The Role of Micelle Size in Tumor Accumulation, Penetration, and Treatment

机译:胶束大小在肿瘤积累,穿透和治疗中的作用

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The specific sizes that determine optimal nanoparticle tumor accumulation, penetration, and treatment remain inconclusive because many studies compared nanoparticles with multiple physicochemical variables (e.g., chemical structures, shapes, and other physical properties) in addition to the size. In this study, we synthesized amphiphilic block copolymers of 7-ethyl-10-hydroxylcamptothecin (SN38) prodrug and fabricated micelles with sizes ranging from 20 to 300 nm from a single copolymer. The as-prepared micelles had exactly the same chemical structures and similar physical properties except for size, which provided an ideal platform for a systematic investigation of the size effects in cancer drug delivery. We found that the micelle's blood circulation time and tumor accumulation increased with the increase in their diameters, with optimal diameter range of 100 to 160 nm. However, the much higher tumor accumulation of the large micelles (100 nm) did not result in significantly improved therapeutic efficacy, because the large micelles had poorer tumor penetration than the small ones (30 nm). An optimal size that balances drug accumulation and penetration in tumors is critical for improving the therapeutic efficacy of nanoparticulate drugs.
机译:决定最佳纳米颗粒肿瘤聚集,穿透和治疗的具体尺寸仍然没有定论,因为许多研究将纳米颗粒除尺寸之外还具有多种物理化学变量(例如化学结构,形状和其他物理性质)。在这项研究中,我们合成了7-乙基-10-羟基喜树碱(SN38)前药的两亲嵌段共聚物,并从单个共聚物制备了尺寸范围为20至300 nm的胶束。所制备的胶束除大小外具有完全相同的化学结构和相似的物理性质,这为系统研究癌症药物递送中的大小效应提供了理想的平台。我们发现,胶束的血液循环时间和肿瘤积累随着直径的增加而增加,最佳直径范围为100至160 nm。但是,大胶束(100 nm)的更高的肿瘤蓄积率并未导致治疗效果的显着提高,因为大胶束的肿瘤渗透性比小胶束(30 nm)差。平衡药物在肿瘤中的积累和渗透的最佳尺寸对于提高纳米颗粒药物的治疗功效至关重要。

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