Bioorganic investigation of encapsulated Cysteine derivative into polymeric nanocarrier

Ehab M. M. Ali, A. Hamed
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引用次数: 1

Abstract

In this work, the copolymer-based synthesized Cysteine-loaded nanocarriers prepared by a routine protocol, coprecipitation method. It is the first report to investigate the neuroprotective potential and biocompatibility of Cysteine derivatives loaded into poly(ethylene glycol)-block-poly(e−caprolactone) methyl ether (PEG-b-PCL). The average size of the polymeric/empty NCs was 89 nm and for polymeric/Synthesized derivative of Cysteine was 126 nm. The Drug Loading efficiency was 81%. The concentration of Polymeric NCs was 2.1 x 10 10 particles/ml and the zeta potential of polymeric/empty and polymeric/ Synthesized derivative of Cysteine NCs -5 mV and -11 mV respectively. Biological part of this work were investigated in the SH-SY5Y human neuroblastoma cell line using cell viability and toxicity assays. The concentration of polymeric NCs below 1 x 10 10 particles/ml described as a zero-point damageable for the cell line. Also the Synthesized derivative of Cysteine encapsulated into polymeric NCs have more neuroprotective effect compared to free Cysteine at lower concentration, and therefore, have a significant neuroprotective potential against Z-VAD-fmk and St-evoked SH-SY5Y cell damage.
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半胱氨酸衍生物包封聚合物纳米载体的生物有机研究
本论文采用共沉淀法合成了基于共聚物的半胱氨酸负载纳米载体。这是第一个研究半胱氨酸衍生物负载到聚乙二醇-嵌段聚(e -己内酯)甲基醚(PEG-b-PCL)中的神经保护潜力和生物相容性的报告。聚合物/空NCs的平均尺寸为89 nm,聚合物/半胱氨酸合成衍生物的平均尺寸为126 nm。载药效率为81%。聚合物NCs的浓度为2.1 × 10 10粒/ml,聚合物/空半胱氨酸NCs和聚合物/合成半胱氨酸NCs衍生物的ζ电位分别为-5 mV和-11 mV。本研究的生物学部分在SH-SY5Y人神经母细胞瘤细胞系中进行了细胞活力和毒性试验。聚合物nc的浓度低于1 × 1010颗粒/ml,称为细胞系的零点损伤。与低浓度的游离半胱氨酸相比,聚合NCs包封的半胱氨酸衍生物具有更强的神经保护作用,因此对Z-VAD-fmk和st诱发的SH-SY5Y细胞损伤具有显著的神经保护潜力。
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