Gene Transfer Technology Group, Institute for Women's Health, University College London, 86-96 Chenies Mews, London, WC1E 6HX, UK.
FASEB J. 2011 Oct;25(10):3505-18. doi: 10.1096/fj.11-182311. Epub 2011 Jul 11.
Several diseases of the nervous system are characterized by neurodegeneration and death in childhood. Conventional medicine is ineffective, but fetal or neonatal gene therapy may provide an alternative route to treatment. We evaluated the ability of single-stranded and self-complementary adeno-associated virus pseudotype 2/9 (AAV2/9) to transduce the nervous system and target gene expression to specific neural cell types following intravenous injection into fetal and neonatal mice, using control uninjected age-matched mice. Fetal and neonatal administration produced global delivery to the central (brain, spinal cord, and all layers of the retina) and peripheral (myenteric plexus and innervating nerves) nervous system but with different expression profiles within the brain; fetal and neonatal administration resulted in expression in neurons and protoplasmic astrocytes, respectively. Neither single-stranded nor self-complementary AAV2/9 triggered a microglia-mediated immune response following either administration. In summary, intravenous AAV2/9 targets gene expression to specific neural cell types dependent on developmental stage. This represents a powerful tool for studying nervous system development and disease. Furthermore, it may provide a therapeutic strategy for treatment of early lethal genetic diseases, such as Gaucher disease, and for disabling neuropathies, such as preterm brain injury.
几种神经系统疾病的特征是儿童期神经退行性变和死亡。传统医学无效,但胎儿或新生儿基因治疗可能提供一种替代治疗途径。我们评估了单链和自互补腺相关病毒假型 2/9(AAV2/9)在通过静脉内注射到胎儿和新生小鼠后,穿过血脑屏障向特定神经细胞类型转导和靶向基因表达的能力,使用对照未注射的同龄匹配小鼠。胎儿和新生儿给药导致中枢神经系统(脑、脊髓和视网膜的所有层)和外周神经系统(肌间神经丛和支配神经)的全身传递,但在脑内具有不同的表达谱;胎儿和新生儿给药分别导致神经元和原浆星形胶质细胞的表达。单链和自互补 AAV2/9 均未在两种给药途径后引发小胶质细胞介导的免疫反应。总之,静脉内 AAV2/9 依赖于发育阶段将基因表达靶向特定的神经细胞类型。这代表了研究神经系统发育和疾病的强大工具。此外,它可能为治疗早期致死性遗传疾病(如戈谢病)和致残性神经病(如早产儿脑损伤)提供治疗策略。
