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首页> 外文期刊>Journal of biomedical materials research, Part A >Amphiphilic Y shaped miktoarm star copolymer for anticancer hydrophobic and hydrophilic drugs codelivery: Synthesis, characterization, in vitro in vitro , and in vivo in vivo biocompatibility study
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Amphiphilic Y shaped miktoarm star copolymer for anticancer hydrophobic and hydrophilic drugs codelivery: Synthesis, characterization, in vitro in vitro , and in vivo in vivo biocompatibility study

机译:Amphiphilic Y成型Miktoarm StartoMar共聚物抗癌疏水和亲水药物编码:合成,表征,体外体外体外,体内体内生物相容性研究

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Abstract In this project, a core‐shell polymersome based on miktoarm star‐copolymer:methoxy poly‐ethylene glycol‐lysine‐(poly‐caprolactone) 2 was synthesized by a new method as controlled targeted drug delivery systems for codelivery of the chemotherapeutic methotrexate (MTX) and curcumin (CUR). Some properties of these nanocarriers (NCs), such as surface morphology, structure, surface charge, stability, and biocompatibility, were evaluated by proton nuclear magnetic resonance, dynamic scanning colorimetry, Fourier‐transform infrared spectroscopy, dynamic light scattering, atomic force microscopy, critical aggregation concentration, hemolysis test, MTT assay, and lethal dose 50 (LD50). The AFM results showed that the uniform spherical morphology of NCs have an average size of about ~60?nm. The drug loading of NCs was about 14.13 and 10.93% for CUR and MTX, respectively. The NCs revealed pH‐sensitivity in drug release. The release of drugs from miktoarm‐based NCs in neutral pH was lower than in acidic medium because of faster degradation of polymersome in acidic environment. MTT assay results showed that the drug‐loaded NCs did not show significant toxicity due to which cell viability maintain over 82% at 300?μg/mL concentration. Also, synthesized miktoarm showed hemolysis lower than 3%. This result was repeated in LD50, and all mice which treat with 5000?mg/kg were still alive after 24?h. These result confirmed safety of miktoarm star copolymer. Eventually, the goal of this study is the application of water‐soluble star copolymers miktoarm with pH dependent release properties for designing a new drug delivery carrier and using CUR for enhancing anticancer properties of MTX. ? 2018 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 106A: 2817–2826, 2018.
机译:摘要在该项目中,通过新方法合成了基于MikoThar-Copolymer的核 - 壳聚合物:甲氧基聚乙二醇 - 赖氨酸 - (聚己内酯)2,作为用于化学治疗甲氨蝶呤的CodeLivery的靶向药物递送系统( mtx)和姜黄素(cur)。通过质子核磁共振评估这些纳米载波(NCS)的一些性质,例如表面形态,结构,表面电荷,稳定性和生物相容性,动态扫描比色法,傅立叶变换红外光谱,动态光散射,原子力显微镜,临界聚集浓度,溶血试验,MTT测定和致死剂量50(LD50)。 AFM结果表明,NCS的均匀球形形态的平均尺寸约为约〜60Ω。对于Cur和MTX,NC的药物负荷分别为约14.13和10.93%。 NCS揭示了药物释放中的pH敏感性。由于酸性环境中的聚合物的较快降解,来自中性pH基于Miktoarm的NCS的药物释放的中性pH值低于酸性介质。 MTT测定结果表明,由于在300μg/ ml浓度下,该药物负载的NCs未显示出显着的毒性。此外,合成的Miktoarm表现出低于3%的溶血。该结果在LD50重复,并在24μm后处理5000μg/ kg的所有小鼠仍然活着。这些结果证实了Miktoarm Star共聚物的安全性。最终,本研究的目的是应用水溶性星形共聚物MiktoArm与pH依赖性释放性质,用于设计新的药物递送载体并使用Cur用于增强MTX的抗癌性质。还2018 Wiley期刊,Inc.J生物保解员A部分:106A:2817-2826,2018。

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