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Organically modified silica nanoparticles: A nonviral vector for in vivo gene delivery and expression in the brain

机译:有机修饰的二氧化硅纳米颗粒:一种非病毒载体用于体内基因传递和在大脑中表达

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摘要

This article reports on the application of organically modified silica (ORMOSIL) nanoparticles as a nonviral vector for efficient in vivo gene delivery. Highly monodispersed, stable aqueous suspension of nanoparticles, surface-functionalized with amino groups for binding of DNA, were prepared and characterized. Stereotaxic injections of nanoparticles, complexed with plasmid DNA encoding for EGFP, into the mouse ventral midbrain and into lateral ventricle, allowed us to fluorescently visualize the extensive transfection of neuronal-like cells in substantia nigra and areas surrounding the lateral ventricle. No ORMOSIL-based toxicity was observed 4 weeks after transfection. The efficiency of transfection equaled or exceeded that obtained in studies using a viral vector. An in vivo optical imaging technique (a fiber-based confocal fluorescent imaging system) provided an effective means to show the retention of viability of the transfected cells. The ORMOSIL-mediated transfections also were used to manipulate the biology of the neural stem/progenitor cells in vivo. Transfection of a plasmid expressing the nucleus-targeting fibroblast growth factor receptor type 1 resulted in significant inhibition of the in vivo incorporation of bromodeoxyuridine into the DNA of the cells in the subventricular zone and the adjacent rostral migratory stream. This in vivo approach shows that the nuclear receptor can control the proliferation of the stem/progenitor cells in this region of the brain. The results of this nanomedicine approach using ORMOSIL nanoparticles as a nonviral gene delivery platform have a promising future direction for effective therapeutic manipulation of the neural stem/progenitor cells as well as in vivo targeted brain therapy.
机译:本文报道了有机修饰的二氧化硅(ORMOSIL)纳米粒子作为非病毒载体有效体内基因传递的应用。制备并表征了高度单分散,稳定的纳米颗粒水悬浮液,该表面经氨基表面官能化以与DNA结合。纳米粒的立体定向注射,与编码EGFP的质粒DNA复合,进入小鼠腹中脑和侧脑室,使我们能够荧光可视化黑质和侧脑室周围区域神经元样细胞的广泛转染。转染后4周未观察到基于ORMOSIL的毒性。转染效率等于或超过使用病毒载体进行的研究中获得的效率。体内光学成像技术(基于纤维的共聚焦荧光成像系统)提供了一种有效的手段来显示转染细胞的活力。 ORMOSIL介导的转染也被用来在体内操纵神经干/祖细胞的生物学。转染表达1型靶向核成纤维细胞生长因子受体的质粒导致显着抑制溴脱氧尿苷在体内掺入到脑室下区域和邻近的鼻端迁徙流中的细胞DNA中。这种体内方法显示核受体可以控制脑部该区域中干/祖细胞的增殖。使用ORMOSIL纳米颗粒作为非病毒基因递送平台的这种纳米医学方法的结果,对于神经干/祖细胞的有效治疗操作以及体内靶向性脑治疗具有广阔的未来方向。

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