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Engineered AAVs for efficient noninvasive gene delivery to the central and peripheral nervous systems

机译:工程化的AAV可将无创基因有效地传递到中枢和周围神经系统

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摘要

Adeno-associated viruses (AAVs) are commonly used for in vivo gene transfer. Nevertheless, AAVs that provide efficient transduction across specific organs or cell populations are needed. Here, we describe AAV-PHP.eB and AAV-PHP.S, capsids that efficiently transduce the central and peripheral nervous systems, respectively. In the adult mouse, intravenous administration of 1 × 1011 vector genomes (vg) of AAV-PHP.eB transduced 69% of cortical and 55% of striatal neurons, while 1 × 1012 vg of AAV-PHP.S transduced 82% of dorsal root ganglion neurons, as well as cardiac and enteric neurons. The efficiency of these vectors facilitates robust cotransduction and stochastic, multicolor labeling for individual cell morphology studies. To support such efforts, we provide methods for labeling a tunable fraction of cells without compromising color diversity. Furthermore, when used with cell-type-specific promoters and enhancers, these AAVs enable efficient and targetable genetic modification of cells throughout the nervous system of transgenic and non-transgenic animals.
机译:腺相关病毒(AAV)通常用于体内基因转移。尽管如此,仍需要能够在特定器官或细胞群体之间提供有效转导的AAV。在这里,我们描述了AAV-PHP.eB和AAV-PHP.S衣壳,它们分别有效地转导中枢神经系统和周围神经系统。在成年小鼠中,静脉内注射1×1011 vg AAV-PHP.eB基因组可转导69%的皮质和55%的纹状体神经元,而1×1012 vg AAV-PHP.S则可转导背侧的82%。根神经节神经元,以及心脏和肠神经元。这些载体的效率促进了针对单个细胞形态学研究的稳健的共转导和随机多色标记。为支持此类工作,我们提供了在不影响颜色多样性的情况下标记细胞可调部分的方法。此外,当与细胞类型特异性启动子和增强子一起使用时,这些AAV可在整个转基因和非转基因动物的神经系统中对细胞进行有效且可靶向的遗传修饰。

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