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首页> 外文期刊>RSC Advances >The non-innocent nature of graphene oxide as a theranostic platform for biomedical applications and its reactivity towards metal-based anticancer drugs
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The non-innocent nature of graphene oxide as a theranostic platform for biomedical applications and its reactivity towards metal-based anticancer drugs

机译:氧化石墨烯作为生物医学应用的治疗学平台的非清白性质及其对基于金属的抗癌药的反应性

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摘要

The self-assembly process in a solution of a mononuclear iron(II) complex based on the bispyrazolylpyridine scaffold with graphene oxide (GO) micrometer-sheets allows not only the devising of a new hybrid-architecture for GO-based materials suitable for nanomedicine, but also the unveiling of the reactive nature of GO as a drug-carrier. The neat iron complex is found to be highly active in disrupting the cell cycle through DNA binding, with behaviour and efficiency similar to that expressed by ruthenium-complexes as well as antibiotic-drugs such as doxorubicin. On the contrary, in the hybrid material the proclivity of neat GO to produce reactive oxygen species (ROS) became down-regulated by the electron-buffering properties of the loaded iron complex, evidencing the presence of an active electron transfer from the drug to GO. These findings question the use of the neat GO platform as a suitable carrier for metal-based anticancer drugs and highlight the importance of addressing the chemical/physical integrity of the drug being loaded into GO before drawing conclusions on the potential effectiveness of the hybrid material for medical applications.
机译:在基于双吡唑基吡啶骨架和氧化石墨烯(GO)微米片的单核铁(II)配合物溶液中的自组装过程,不仅可以为适用于纳米药物的GO基材料设计新的混合体系结构,还揭示了GO作为药物载体的反应性。发现纯铁络合物在通过DNA结合破坏细胞周期中具有很高的活性,其行为和效率与钌络合物以及抗生素药物(如阿霉素)所表达的相似。相反,在杂化材料中,纯净的GO产生活性氧(ROS)的倾向性被负载的铁络合物的电子缓冲性能下调,证明存在从药物到GO的活性电子转移。这些发现质疑使用纯净的GO平台作为金属基抗癌药物的合适载体,并强调了在得出杂化材料对人体的潜在效力的结论之前,应对加载到GO中的药物的化学/物理完整性的重要性。医疗应用。

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