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A brief review of reporter gene imaging in oncolytic virotherapy and gene therapy

机译:浅谈Collytic病毒疗法和基因治疗中的报告基因成像

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Reporter gene imaging (RGI) can accelerate development timelines for gene and viral therapies by facilitating rapid and noninvasive in?vivo studies to determine the biodistribution, magnitude, and durability of viral gene expression and/or virus infection. Functional molecular imaging systems used for this purpose can be divided broadly into deep-tissue and optical modalities. Deep-tissue modalities, which can be used in animals of any size as well as in human subjects, encompass single photon emission computed tomography (SPECT), positron emission tomography (PET), and functional/molecular magnetic resonance imaging (f/mMRI). Optical modalities encompass fluorescence, bioluminescence, Cerenkov luminescence, and photoacoustic imaging and are suitable only for small animal imaging. Here we discuss the mechanisms of action and relative merits of currently available reporter gene systems, highlighting the strengths and weaknesses of deep tissue versus optical imaging systems and the hardware/reagents that are used for data capture and processing. In light of recent technological advances, falling costs of imaging instruments, better availability of novel radioactive and optical tracers, and a growing realization that RGI can give invaluable insights across the entire in?vivo translational spectrum, the approach is becoming increasingly essential to facilitate the competitive development of new virus- and gene-based drugs.
机译:记者基因成像(RGI)可以通过促进快速和非侵入性,加速基因和病毒疗法的发育时间表,以确定病毒基因表达和/或病毒感染的生物分布,幅度和耐久性。用于此目的的功能分子成像系统可以广泛地分成深组织和光学模式。深组织方式,可用于任何尺寸和人类受试者的动物,包括单光子发射计算机断层扫描(SPECT),正电子发射断层扫描(PET)和功能/分子磁共振成像(F / MMRI) 。光学模式包括荧光,生物发光,Cerenkov发光和光声成像,并且仅适用于小动物成像。在这里,我们讨论目前可用的报告基因系统的行动和相对优点的机制,突出了深组与光学成像系统的强度和弱点以及用于数据捕获和处理的硬件/试剂。鉴于最近的技术进步,成像仪器的下降成本,更好的新颖的放射性和光学示踪剂,以及RGI可以在整个整体中能够在整个方面提供宝贵的洞察力,这一方法变得越来越重要,以方便竞争发展新病毒和基因毒性药物。

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