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Development of Novel Zn2+ Loaded NanoparticlesDesigned for Cell-Type Targeted Drug Release in CNS Neurons: In VitroEvidences

机译:新型负载Zn2 +的纳米粒子的开发设计用于CNS神经元中的细胞类型靶向药物释放:体外证据

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摘要

Intact synaptic function and plasticity are fundamental prerequisites to a healthy brain. Therefore, synaptic proteins are one of the major targets for drugs used as neuro-chemical therapeutics. Unfortunately, the majority of drugs is not able to cross the blood–brain barrier (BBB) and is therefore distributed within the CNS parenchyma. Here, we report the development of novel biodegradable Nanoparticles (NPs), made of poly-lactide-co-glycolide (PLGA) conjugated with glycopeptides that are able to cross the BBB and deliver for example Zn2+ ions. We also provide a thorough characterization of loaded and unloaded NPs for their stability, cellular uptake, release properties, toxicity, and impact on cell trafficking. Our data reveal that these NPs are biocompatible, and can be used to elevate intracellular levels of Zn2+. Importantly, by engineering the surface of NPs with antibodies against NCAM1 and CD44, we were able to selectively target neurons or glial cells, respectively. Our results indicate that these biodegradable NPs provide a potential new venue for the delivery Zn2+ to the CNS and thus a means to explore the influence of altered zinc levels linked to neuropsychological disorders such as depression.
机译:完整的突触功能和可塑性是健康大脑的基本前提。因此,突触蛋白是用作神经化学疗法的药物的主要靶标之一。不幸的是,大多数药物不能穿过血脑屏障(BBB),因此分布在CNS实质内。在这里,我们报告了新型的可生物降解的纳米粒子(NPs)的开发,该纳米粒子由共轭糖肽的聚丙交酯-共-乙交酯(PLGA)制成,能够穿过BBB并传递例如Zn 2 + 离子。我们还提供了已加载和未加载的NP的稳定性,细胞摄取,释放特性,毒性以及对细胞运输的影响的全面表征。我们的数据表明,这些NP具有生物相容性,可用于提高细胞内Zn 2 + 的水平。重要的是,通过用针对NCAM1和CD44的抗体改造NP的表面,我们能够分别选择性地靶向神经元或神经胶质细胞。我们的结果表明,这些可生物降解的NPs为将Zn 2 + 输送到中枢神经系统提供了潜在的新场所,因此是探索锌水平变化与神经心理疾病(例如抑郁症)相关的影响的手段。

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