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首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Synthesis, characterization and in vitro evaluation of novel vitamin D3 nanoparticles as a versatile platform for drug delivery in cancer therapy
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Synthesis, characterization and in vitro evaluation of novel vitamin D3 nanoparticles as a versatile platform for drug delivery in cancer therapy

机译:新型维生素D3纳米颗粒的合成,表征和体外评估,作为癌症治疗中药物输送的多功能平台

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Development of novel nanotechnology based platforms can impact cancer therapeutics in a paradigm shifting manner. The major concerns in drug delivery in cancer therapy are the biocompatibility, biodegradability, non-toxic nature, easy and short synthesis and versatility of the nanovectors. Herein we report the engineering of versatile nanoparticles from biocompatible, biodegradable and non-toxic lipid soluble vitamin D3. We have conjugated different clinically used cytotoxic drugs (paclitaxel and doxorubicin) as well as PI3 kinase inhibitor (PI103) with vitamin D3 using a succinic acid linker. Sub-200 nm, mono-dispersed nanoparticles with high drug loading were engineered from the vitamin D3-succinic acid-drug conjugates. These nanoparticles released the active drugs at pH 5.5 in a slow and sustained manner over 100 h. Furthermore, these nanoparticles were taken up by HeLa cells into the low pH lysosomal compartments through an endocytosis mechanism in 6 h. Finally, these drug loaded vitamin D3 nanoparticles induced HeLa cervical cancer cell death in a dose dependent manner at 48 h to show their potential in cancer therapeutics.
机译:基于纳米技术的新型平台的开发可以以范式转移的方式影响癌症治疗。癌症治疗中药物递送的主要问题是纳米载体的生物相容性,生物降解性,无毒性质,容易和短时间合成以及多功能性。在这里,我们报道了从生物相容性,可生物降解的和无毒的脂溶性维生素D3多功能纳米颗粒的工程。我们使用琥珀酸接头将不同的临床使用的细胞毒性药物(紫杉醇和阿霉素)以及PI3激酶抑制剂(PI103)与维生素D3结合在一起。用维生素D3-琥珀酸-药物偶联物设计了具有高载药量的低于200 nm的单分散纳米颗粒。这些纳米粒子在100小时内以缓慢且持续的方式在pH 5.5释放活性药物。此外,这些纳米颗粒在6小时内通过内吞作用被HeLa细胞吸收到低pH溶酶体区室中。最后,这些载有药物的维生素D3纳米颗粒在48小时以剂量依赖的方式诱导HeLa宫颈癌细胞死亡,显示出它们在癌症治疗中的潜力。

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