首页> 美国卫生研究院文献>Molecular Therapy >In Vivo Selection of a Computationally Designed SCHEMA AAV Library Yields a Novel Variant for Infection of Adult Neural Stem Cells in the SVZ
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In Vivo Selection of a Computationally Designed SCHEMA AAV Library Yields a Novel Variant for Infection of Adult Neural Stem Cells in the SVZ

机译:在通过计算设计的SCHEMA AAV库进行的重要选择中产生了一种感染SVZ中成人神经干细胞的新型变体

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摘要

Directed evolution continues to expand the capabilities of complex biomolecules for a range of applications, such as adeno-associated virus vectors for gene therapy; however, advances in library design and selection strategies are key to develop variants that overcome barriers to clinical translation. To address this need, we applied structure-guided SCHEMA recombination of the multimeric adeno-associated virus (AAV) capsid to generate a highly diversified chimeric library with minimal structural disruption. A stringent in vivo Cre-dependent selection strategy was implemented to identify variants that transduce adult neural stem cells (NSCs) in the subventricular zone. A novel variant, SCH9, infected 60% of NSCs and mediated 24-fold higher GFP expression and a 12-fold greater transduction volume than AAV9. SCH9 utilizes both galactose and heparan sulfate as cell surface receptors and exhibits increased resistance to neutralizing antibodies. These results establish the SCHEMA library as a valuable tool for directed evolution and SCH9 as an effective gene delivery vector to investigate subventricular NSCs.
机译:定向进化继续扩展了复杂生物分子在各种应用中的能力,例如用于基因治疗的腺相关病毒载体。然而,图书馆设计和选择策略的进步对于开发克服临床翻译障碍的变体至关重要。为了满足这一需求,我们应用了多聚腺相关病毒(AAV)衣壳的结构指导的SCHEMA重组,以产生高度多样化的嵌合文库,并将结构破坏降至最低。实施了严格的体内Cre依赖性选择策略,以识别在脑室下区域转导成年神经干细胞(NSC)的变体。新型变体SCH9感染了60%的NSC,并介导了比AAV9高24倍的GFP表达和12倍的转导量。 SCH9同时利用半乳糖和硫酸乙酰肝素作为细胞表面受体,并表现出对中和抗体的增强抗性。这些结果将SCHEMA文库确立为用于定向进化的有价值工具,并将SCH9建立为研究脑室下NSC的有效基因传递载体。

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