Fibril-shaped aggregates of doxorubicin with poly-l-lysine and its derivative
文献信息
Feiyan Zhu, Yongri Liang, Fuxin Liang, Qian Wang, Jiaoli Li, Zhibo Li, Zhenzhong Yang
Complex formation between polymers and organic molecules is an interesting topic in polymer physics. Compared to the influence of small molecules on polymer assembly, there are fewer examples demonstrating the effect of polymers on the supramolecular structures formed by organic molecules. In this paper, we first prove that doxorubicin (DOX), a common anti-tumour drug, assembles into fibril-like aggregates in phosphate buffer (pH 7.4) and then show that the assembly of DOX was influenced by the complexation with an amphiphilic poly (amino acid) derivative, i.e. cholate-grafted poly-L-lysine (PLL-CA). With PLL-CA, the DOX fibrils converted to helix structured nano-spindles, whilst the presence of PLL led to minor change on the morphology of PLL/DOX complex compared to the DOX aggregates, which is attributed to the amplitude of intermolecular interactions. As a DNA intercalating agent, the aggregation of DOX on its biofunctionality was also investigated, showing that the formation of fibril assemblies was unfavourable for the cellular internalization of DOX and caused lower cytotoxicity to DOX resistance MCF-7 cells, whereas the polymer/DOX complexes gained an improved cell uptake on the MCF-7/ADR cell line due to an enhanced electrostatic interaction between the complexes and the cell membrane.
期刊推荐

Russian Journal of Bioorganic Chemistry

Saudi Pharmaceutical Journal

Chemical Communications

Drug Discovery Today

Russian Journal of General Chemistry

Nature Medicine

Organic Process Research & Development

Journal of Natural Medicines

Russian Journal of Coordination Chemistry

Journal of Saudi Chemical Society
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Polymer Chemistry

Polymer Chemistry welcomes submissions in all areas of polymer science that have a strong focus on macromolecular chemistry. Manuscripts may cover a broad range of fields, yet no direct application focus is required.
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