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首页> 外文期刊>Clinical chemistry and laboratory medicine: CCLM >Ribozyme gene therapy for autosomal dominant retinal disease.
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Ribozyme gene therapy for autosomal dominant retinal disease.

机译:核酶基因治疗常染色体显性视网膜疾病。

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Gene delivery to cells of the retina, particularly to photoreceptor cells, has broad potential both for answering basic questions of retinal biology and for more applied therapeutic purposes. The use of ribozymes as therapy for autosomal dominant retinal diseases is a promising technique, and the theoretical and practical basis for their use is discussed. The process involves designing and testing ribozymes first in vitro and then in animal models of retinal disease. Viral vectors based on the nonpathogenic human adeno-associated virus, when coupled with the strong, rod photoreceptor specific opsin promoter, offer an efficient and nontoxic way to deliver and express ribozymes in photoreceptor cells for long time periods of time. Effective ribozyme-mediated therapy also demands careful in vitro analysis of a ribozyme's ability to efficiently and specifically distinguish between mutant and wild type RNAs. Finally, effective demonstration of therapy in an animal model requires careful analysis of any rescue effect in the retina using multiple criteria, including biochemical, structural and physiological assays. For this purpose, ribozyme therapy in a transgenic rat model of retinitis pigmentosa containing a dominant rod opsin mutation (proline-to-histidine change at position 23) is discussed in detail.
机译:基因传递到视网膜细胞,特别是光感受器细胞,在回答视网膜生物学基本问题和更广泛的治疗目的方面都具有广阔的潜力。核酶作为常染色体显性遗传性视网膜疾病的治疗方法是有前途的技术,并讨论了其应用的理论和实践基础。该过程涉及首先在体外设计和测试核酶,然后在视网膜疾病的动物模型中进行设计。基于非致病性人腺相关病毒的病毒载体,与强的棒状光感受器特异性视蛋白启动子结合时,可提供一种有效且无毒的方式,可长时间长时间在光感受器细胞中传递和表达核酶。有效的核酶介导的疗法还需要对核酶有效,特异地区分突变型和野生型RNA的能力进行仔细的体外分析。最后,要在动物模型中进行有效的治疗演示,就需要使用多种标准仔细分析视网膜中的任何挽救效果,包括生物化学,结构和生理分析。为此,将详细讨论在色素性视网膜炎转基因大鼠模型中的核酶治疗,该模型包含显性视杆视蛋白突变(脯氨酸到组氨酸在位置23发生变化)。

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