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Imaging Herpes Simplex Virus Type 1 Amplicon Vector-Mediated Gene Expression in Human Glioma Spheroids

机译:成像人类胶质瘤球体中单纯疱疹病毒1型扩增子载体介导的基因表达。

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Vectors derived from herpes simplex virus type 1 (HSV-1) have great potential for transducing therapeutic genes into the central nervous system; however, inefficient distribution of vector particles in vivo may limit their therapeutic potential in patients with gliomas. This study was performed to investigate the extent of HSV-1 amplicon vector-mediated gene expression in a three-dimensional glioma model of multicellular spheroids by imaging highly infectious HSV-1 virions expressing green fluorescent protein (HSV-GFP). After infection or microscopy-guided vector injection of glioma spheroids at various spheroid sizes, injection pressures and injection times, the extent of HSV-1 vector-mediated gene expression was investigated via laser scanning microscopy. Infection of spheroids with HSV-GFP demonstrated a maximal depth of vector-mediated GFP expression at 70 to 80 |im. A > 80% transduction efficiency was reached only in small spheroids with a diameter of < 150 (im. Guided vector injection into the spheroids showed transduction efficiencies ranging between < 10 and > 90%. The results demonstrated that vector-mediated gene expression in glioma spheroids was strongly dependent on the mode of vector application—injection pressure and injection time being the most important parameters. The assessment of these vector application parameters in tissue models will contribute to the development of safe and efficient gene therapy protocols for clinical application.
机译:源自1型单纯疱疹病毒(HSV-1)的载体具有将治疗性基因导入中枢神经系统的巨大潜力。然而,载体颗粒在体内的低效率分布可能会限制其在神经胶质瘤患者中的治疗潜力。通过对表达绿色荧光蛋白(HSV-GFP)的高感染性HSV-1病毒颗粒进行成像,研究了三维细胞胶质瘤三维胶质瘤模型中HSV-1扩增子载体介导的基因表达的程度。在感染或在显微镜引导下以各种球体大小,注射压力和注射时间注射胶质瘤球体的载体后,通过激光扫描显微镜研究了HSV-1载体介导的基因表达的程度。 HSV-GFP感染小球表明,载体介导的GFP表达在70-80μim处最大。只有直径小于150的小球状体才能达到> 80%的转导效率(即,引导载体注射入球状体中,其转导效率介于<10和> 90%之间。结果表明,胶质瘤中介导的基因表达水平球体在很大程度上取决于载体的应用方式,注射压力和注射时间是最重要的参数,在组织模型中对这些载体应用参数的评估将有助于开发安全有效的基因治疗方案以用于临床。

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