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pH-Responsive i-motif Conjugated Hyaluronic Acid/Polyethylenimine Complexes for Drug Delivery Systems

机译:pH响应性i-基序共轭的透明质酸/聚乙烯亚胺复合物用于药物输送系统

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摘要

i-motif is cytosine (C)-rich oligonucleotide (ODN) which shows pH-responsive structure change in acidic condition. Therefore, it has been utilized for the trigger of intercalated drug release, responding to environmental pH change. In this study, 2.76 molecules of i-motif binding ODNs (IBOs) were conjugated to each hyaluronic acid (HA) via amide bond linkages. Synthesis of HA-IBO conjugate (HB) was confirmed by FT-IR and agarose gel electrophoresis with Stains-All staining. After hybridization of HB with i-motif ODN (IMO), it was confirmed that doxorubicin (DOX) could be loaded in HB-IMO hybrid structure (HBIM) with 65.6% of drug loading efficiency (DLE) and 25.0% of drug loading content (DLC). At pH 5.5, prompt and significant DOX release from HBIM was observed due to the disruption of HBIM hybrid structure via i-motif formation of IMO, contrary to pH 7.4 condition. Then, HBIM was complexed with low molecular weight polyethylenimine (PEI1.8k), forming positively charged nanostructures (Z-average size: 126.0 ± 0.4 nm, zeta-potential: 16.1 ± 0.3 mV). DOX-loaded HBIM/PEI complexes displayed higher anticancer efficacy than free DOX in A549 cells, showing the potential for pH-responsive anticancer drug delivery systems.
机译:i-基序是富含胞嘧啶(C)的寡核苷酸(ODN),在酸性条件下显示pH响应结构变化。因此,它已被用于触发嵌入药物释放,以响应环境pH的变化。在这项研究中,通过酰胺键将2.76个i-基序结合ODN(IBO)分子与每个透明质酸(HA)缀合。通过FT-IR和带有Stains-All染色的琼脂糖凝胶电泳证实了HA-IBO缀合物(HB)的合成。 HB与i-motif ODN(IMO)杂交后,证实阿霉素(DOX)可以以HB-IMO杂化结构(HBIM)的形式负载,其载药效率(DLE)为65.6%,载药量为25.0% (DLC)。在pH 5.5下,与pH 7.4条件相反,由于通过IMO的i-基序形成破坏了HBIM杂化结构,导致从HBIM迅速而显着释放DOX。然后,HBIM与低分子量聚乙烯亚胺(PEI1.8k)络合,形成带正电荷的纳米结构(Z平均尺寸:126.0±0.4 nm,ζ电位:16.1±0.3 mV)。载有DOX的HBIM / PEI复合物在A549细胞中显示出比游离DOX更高的抗癌功效,显示了对pH响应的抗癌药物递送系统的潜力。

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