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高纯度的 AAV 载体可导致转导效率与血清型和组织无关的增强。

High AAV vector purity results in serotype- and tissue-independent enhancement of transduction efficiency.

机构信息

Department of Biochemistry and Molecular Biology, Center of Animal Biotechnology and Gene Therapy, School of Veterinary Medicine, Universitat Autònoma de Barcelona, Bellaterra, Spain.

出版信息

Gene Ther. 2010 Apr;17(4):503-10. doi: 10.1038/gt.2009.157. Epub 2009 Dec 3.

Abstract

The purity of adeno-associated virus (AAV) vector preparations has important implications for both safety and efficacy of clinical gene transfer. Early-stage screening of candidates for AAV-based therapeutics ideally requires a purification method that is flexible and also provides vectors comparable in purity and potency to the prospective investigational product manufactured for clinical studies. The use of cesium chloride (CsCl) gradient-based protocols provides the flexibility for purification of different serotypes; however, a commonly used first-generation CsCl-based protocol was found to result in AAV vectors containing large amounts of protein and DNA impurities and low transduction efficiency in vitro and in vivo. Here, we describe and characterize an optimized, second-generation CsCl protocol that incorporates differential precipitation of AAV particles by polyethylene glycol, resulting in higher yield and markedly higher vector purity that correlated with better transduction efficiency observed with several AAV serotypes in multiple tissues and species. Vectors purified by the optimized CsCl protocol were found to be comparable in purity and functional activity to those prepared by more scalable, but less flexible serotype-specific purification processes developed for manufacture of clinical vectors, and are therefore ideally suited for pre-clinical studies supporting translational research.

摘要

腺相关病毒 (AAV) 载体制剂的纯度对临床基因转移的安全性和疗效都有重要影响。对于基于 AAV 的治疗候选物的早期筛选,理想情况下需要一种灵活的纯化方法,该方法提供的载体在纯度和效力方面与为临床研究制造的预期研究产品相当。使用氯化铯 (CsCl) 梯度基方案为不同血清型的纯化提供了灵活性;然而,发现常用的第一代 CsCl 基方案会导致 AAV 载体中含有大量蛋白质和 DNA 杂质,并且在体外和体内的转导效率都较低。在这里,我们描述并表征了一种优化的第二代 CsCl 方案,该方案通过聚乙二醇对 AAV 颗粒进行差异沉淀,从而提高产量,并显著提高载体纯度,与在多种组织和物种中观察到的几种 AAV 血清型的更好转导效率相关。通过优化的 CsCl 方案纯化的载体在纯度和功能活性方面与为临床载体制造开发的更具可扩展性但灵活性较低的特定血清型的纯化过程制备的载体相当,因此非常适合支持转化研究的临床前研究。

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