腺相关病毒
遗传增强
脊髓性肌萎缩
载体(分子生物学)
病毒学
病毒载体
医学
基因传递
生物
不利影响
生物信息学
疾病
基因
重组DNA
病理
遗传学
药理学
作者
Jalish M. Riyad,Thomas Weber
出处
期刊:Gene Therapy
[Springer Nature]
日期:2021-03-03
卷期号:28 (12): 683-696
被引量:49
标识
DOI:10.1038/s41434-021-00243-z
摘要
In the last two decades, recombinant adeno-associated virus has emerged as the most popular gene therapy vector. Recently AAV gene therapy has been approved by the FDA for the treatment of two rare genetic disorders, namely the early childhood blindness disease Leber congenital amaurosis and spinal muscular atrophy (SMA). As is the case for the treatment of SMA, if the AAV vector must be administered systemically, very high vector doses are often required for therapeutic efficacy. But higher vector doses inevitably increase the risk of adverse events. The tragic death of three children in a clinical trial to treat X-linked myotubular myopathy with an AAV vector has thrown this limitation into sharp relief. Regardless of the precise cause(s) that led to the death of the two children, it is critical that we develop better AAV vectors to achieve therapeutic levels of expression with lower vector doses. To transduce successfully a target cell, AAV has to overcome both systemic as well as cellular roadblocks. In this review, we discuss some of the most prominent cellular roadblocks that AAV must get past to deliver successfully its therapeutic payload. We also highlight recent advancements in our knowledge of AAV biology that can potentially be harnessed to improve AAV vector performance and thereby make AAV gene therapy safer.
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