Camptothecin (CPT)-based drugs always undergo the reversible, pH-dependent lactone ring-opening reaction, yielding the inactive but toxic carboxylate form. Self-assembly strategy provides an effective route for preserving their bio-stability. In this article, nano-sized self-assemblies from CPT-based antitumor drugs were simply built up by directly diluting the stock dimethylsulfoxide solutions of (S)-(+)-CPT, (S)-10-hydroxyl camptothecin and carboxylic CPT with water/phosphate-buffered saline solution. Because of their different molecular structures in A-ring or modification on the 20-OH group, CPT self-assembled into helical nano-ribbons, whereas 10-hydroxycamptothecin and carboxylic CPT self-aggregated into flat nano-ribbons and cylindric nano-rods, respectively. Attractively, the self-assembly of CPT-based drugs could occur within 1âmin at a low concentration of 1âÃâ10(-5â)M. Adopting the J-type self-aggregation, self-assemblies were stable in aqueous solution and could effectively protect the CPT-based drugs from hydrolysis, which thereby kept their bioactivity for tumor therapy.
Self-defensive nano-assemblies from camptothecin-based antitumor drugs.
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作者:Qin Si-Yong, Peng Meng-Yun, Rong Lei, Li Bin, Wang Shi-Bo, Cheng Si-Xue, Zhuo Ren-Xi, Zhang Xian-Zheng
| 期刊: | Regenerative Biomaterials | 影响因子: | 8.100 |
| 时间: | 2015 | 起止号: | 2015 Sep;2(3):159-66 |
| doi: | 10.1093/rb/rbv011 | ||
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