基因治疗血友病之旅:我们到了吗?
The gene therapy journey for hemophilia: are we there yet?
机构信息
Children's Hospital of Philadelphia, Philadelphia, PA 19104, USA.
出版信息
Blood. 2012 Nov 29;120(23):4482-7. doi: 10.1182/blood-2012-05-423210. Epub 2012 Jul 24.
Abstract
Since the isolation and characterization of the genes for FVIII and FIX some 30 years ago, a longstanding goal of the field has been development of successful gene therapy for the hemophilias. In a landmark study published in 2011, Nathwani et al demonstrated successful conversion of severe hemophilia B to mild or moderate disease in 6 adult males who underwent intravenous infusion of an adeno-associated viral (AAV) vector expressing factor IX. These 6 subjects have now exhibited expression of FIX at levels ranging from 1% to 6% of normal for periods of > 2 years. This review discusses obstacles that were overcome to reach this goal and the next steps in clinical investigation. Safety issues that will need to be addressed before more widespread use of this approach are discussed. Efforts to extend AAV-mediated gene therapy to hemophilia A, and alternate approaches that may be useful for persons with severe liver disease, who may not be candidates for gene transfer to liver, are also discussed.
摘要
自 30 年前分离和鉴定 FVIII 和 FIX 基因以来,该领域的一个长期目标一直是成功开发用于治疗血友病的基因疗法。在 2011 年发表的一项具有里程碑意义的研究中,Nathwani 等人证明,在接受表达因子 IX 的腺相关病毒 (AAV) 载体静脉输注的 6 名成年男性中,严重的乙型血友病成功转化为轻度或中度疾病。这 6 名受试者现在表现出 FIX 的表达水平在正常水平的 1%至 6%之间,持续时间>2 年。这篇综述讨论了为实现这一目标而克服的障碍以及临床研究的下一步。在更广泛地使用这种方法之前,需要解决安全性问题。还讨论了将 AAV 介导的基因疗法扩展到甲型血友病的努力,以及对于严重肝病患者可能有用的替代方法,这些患者可能不适合肝脏基因转移。
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