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新型腺相关病毒的定向进化用于治疗性基因传递。

Directed evolution of novel adeno-associated viruses for therapeutic gene delivery.

机构信息

Department of Chemical and Biomolecular Engineering, University of California, Berkeley, CA 94720, USA.

出版信息

Gene Ther. 2012 Jun;19(6):694-700. doi: 10.1038/gt.2012.20. Epub 2012 Mar 8.

Abstract

Gene therapy vectors based on adeno-associated virus (AAV) are currently in clinical trials for numerous disease targets, such as muscular dystrophy, hemophilia, Parkinson's disease, Leber's congenital amaurosis and macular degeneration. Despite its considerable promise and emerging clinical success, several challenges impede the broader implementation of AAV gene therapy, including the prevalence of neutralizing antibodies in the human population, low transduction of a number of therapeutically relevant cell and tissue types, an inability to overcome physical and cellular barriers in vivo and a relatively limited carrying capacity. These challenges arise as the demands we place on AAV vectors are often different from or even at odds with the properties nature bestowed on their parent viruses. Viral-directed evolution-the iterative generation of large, diverse libraries of viral mutants and selection for variants with specific properties of interest-offers an approach to address these problems. Here we outline progress in creating novel classes of AAV variant libraries and highlight the successful isolation of variants with novel and advantageous in vitro and in vivo gene delivery properties.

摘要

基于腺相关病毒(AAV)的基因治疗载体目前正在针对多种疾病靶点进行临床试验,例如肌肉营养不良、血友病、帕金森病、莱伯先天性黑矇和黄斑变性。尽管腺相关病毒基因治疗具有很大的潜力并取得了新的临床成功,但仍有几个挑战阻碍了其更广泛的应用,包括在人群中普遍存在中和抗体、许多治疗相关细胞和组织类型的转导效率低、无法克服体内的物理和细胞屏障以及相对有限的承载能力。这些挑战的出现是因为我们对腺相关病毒载体的要求通常与赋予其亲本病毒的特性不同,甚至存在冲突。病毒定向进化——迭代产生大量多样化的病毒突变体文库,并选择具有特定感兴趣特性的变体——为解决这些问题提供了一种方法。在这里,我们概述了创建新型 AAV 变体文库的进展,并强调了成功分离出具有新型和有利的体外和体内基因传递特性的变体。

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