Powell S K, Khan N, Parker C L, Samulski R J, Matsushima G, Gray S J, McCown T J
Gene Therapy Center, Chapel Hill, NC, USA.
Department of Pharmacology, Chapel Hill, NC, USA.
Gene Ther. 2016 Nov;23(11):807-814. doi: 10.1038/gt.2016.62. Epub 2016 Sep 15.
No adeno-associated virus (AAV) capsid has been described in the literature to exhibit a primary oligodendrocyte tropism when a constitutive promoter drives gene expression, which is a significant barrier for efficient in vivo oligodendrocyte gene transfer. The vast majority of AAV vectors, such as AAV1, 2, 5, 6, 8 or 9, exhibit a dominant neuronal tropism in the central nervous system. However, a novel AAV capsid (Olig001) generated using capsid shuffling and directed evolution was recovered after rat intravenous delivery and subsequent capsid clone rescue, which exhibited a >95% tropism for striatal oligodendrocytes after rat intracranial infusion where a constitutive promoter drove gene expression. Olig001 contains a chimeric mixture of AAV1, 2, 6, 8 and 9, but unlike these parental serotypes after intravenous administration Olig001 has very low affinity for peripheral organs, especially the liver. Furthermore, in mixed glial cell cultures, Olig001 exhibits a 9-fold greater binding when compared with AAV8. This novel oligodendrocyte-preferring AAV vector exhibits characteristics that are a marked departure from previously described AAV serotypes.
在文献中尚未描述当组成型启动子驱动基因表达时,有腺相关病毒(AAV)衣壳表现出原发性少突胶质细胞嗜性,这是体内少突胶质细胞基因高效转移的一个重大障碍。绝大多数AAV载体,如AAV1、2、5、6、8或9,在中枢神经系统中表现出主要的神经元嗜性。然而,在大鼠静脉注射并随后进行衣壳克隆拯救后,回收了一种使用衣壳改组和定向进化产生的新型AAV衣壳(Olig001),当组成型启动子驱动基因表达时,在大鼠颅内注射后,该衣壳对纹状体少突胶质细胞表现出>95%的嗜性。Olig001包含AAV1、2、6、8和9的嵌合混合物,但与这些亲本血清型不同,静脉注射后Olig001对周围器官,尤其是肝脏的亲和力非常低。此外,在混合胶质细胞培养物中,与AAV8相比,Olig001的结合力高9倍。这种新型的偏好少突胶质细胞的AAV载体表现出与先前描述的AAV血清型明显不同的特征。
