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Multifunctional stimuli responsive polymer-gated iron and gold-embedded silica nano golf balls: Nanoshuttles for targeted on-demand theranostics

机译:多功能刺激响应性聚合物门控的铁和金镶嵌的二氧化硅纳米高尔夫球:用于定向按需治疗的纳米梭

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摘要

Multi-functional nanoshuttles for remotely targeted and on-demand delivery of therapeutic molecules and imaging to defined tissues and organs hold great potentials in personalized medicine, including precise early diagnosis, efficient prevention and therapy without toxicity. Yet, in spite of 25 years of research, there are still no such shuttles available. To this end, we have designed magnetic and gold nanoparticles (NP)-embedded silica nanoshuttles (MGNSs) with nanopores on their surface. Fluorescently labeled Doxorubicin (DOX), a cancer drug, was loaded in the MGNSs as a payload. DOX loaded MGNSs were encapsulated in heat and pH sensitive polymer P(NIPAM-co-MAA) to enable controlled release of the payload. Magnetically-guided transport of MGNSs was examined in: (a) a glass capillary tube to simulate their delivery via blood vessels; and (b) porous hydrogels to simulate their transport in composite human tissues, including bone, cartilage, tendon, muscles and blood–brain barrier (BBB). The viscoelastic properties of hydrogels were examined by atomic force microscopy (AFM). Cellular uptake of DOX-loaded MGNSs and the subsequent pH and temperature-mediated release were demonstrated in differentiated human neurons derived from induced pluripotent stem cells (iPSCs) as well as epithelial HeLa cells. The presence of embedded iron and gold NPs in silica shells and polymer-coating are supported by SEM and TEM. Fluorescence spectroscopy and microscopy documented DOX loading in the MGNSs. Time-dependent transport of MGNSs guided by an external magnetic field was observed in both glass capillary tubes and in the porous hydrogel. AFM results affirmed that the stiffness of the hydrogels model the rigidity range from soft tissues to bone. pH and temperature-dependent drug release analysis showed stimuli responsive and gradual drug release. Cells’ viability MTT assays showed that MGNSs are non-toxic. The cell death from on-demand DOX release was observed in both neurons and epithelial cells even though the drug release efficiency was higher in neurons. Therefore, development of smart nanoshuttles have significant translational potential for controlled delivery of theranostics’ payloads and precisely guided transport in specified tissues and organs (for example, bone, cartilage, tendon, bone marrow, heart, lung, liver, kidney, and brain) for highly efficient personalized medicine applications.
机译:用于将治疗分子远程靶向和按需递送以及向定义的组织和器官成像的多功能纳米梭在个性化医学中具有巨大潜力,包括精确的早期诊断,有效的预防和无毒治疗。然而,尽管进行了25年的研究,仍然没有此类航天飞机可用。为此,我们设计了嵌入磁性和金纳米颗粒(NP)的二氧化硅纳米梭(MGNSs),它们的表面具有纳米孔。荧光标记的阿霉素(DOX)(一种抗癌药物)作为有效载荷被装载到MGNS中。将装有DOX的MGNS封装在对热和pH敏感的聚合物P(NIPAM-co-MAA)中,以实现有效载荷的受控释放。在以下方面检查了MGNS的磁导运输:(a)玻璃毛细管模拟通过血管的递送。 (b)多孔水凝胶,以模拟它们在复合人体组织中的运输,包括骨骼,软骨,肌腱,肌肉和血脑屏障(BBB)。通过原子力显微镜(AFM)检查水凝胶的粘弹性质。在衍生自诱导多能干细胞(iPSC)以及上皮HeLa细胞的分化人类神经元中,证明了DOX加载的MGNS的细胞摄取以及随后的pH和温度介导的释放。 SEM和TEM支持在二氧化硅外壳和聚合物涂层中嵌入铁和金NP的存在。荧光光谱法和显微术记录了MGNS中的DOX负载。在玻璃毛细管和多孔水凝胶中均观察到了受外部磁场引导的MGNS的时间依赖性运输。原子力显微镜的结果证实,水凝胶的刚度可以模拟从软组织到骨骼的刚度范围。 pH和温度依赖性药物释放分析显示刺激响应和逐渐释放药物。细胞的MTT生存力分析表明MGNS是无毒的。尽管在神经元中药物释放效率较高,但在神经元和上皮细胞中均观察到了按需DOX释放引起的细胞死亡。因此,开发智能纳米穿梭机具有巨大的翻译潜力,可用于控制治疗药物的有效载荷的输送,并在特定的组织和器官(例如骨骼,软骨,肌腱,骨髓,心脏,肺,肝,肾和脑)中进行精确引导的运输用于高效的个性化医学应用。

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