Monitoring for liver cancer post-gene therapy—How much and how often?

IF 2.5 3区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY
Ype P. de Jong, Ira M. Jacobson
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引用次数: 0

Abstract

Hepatocellular carcinoma (HCC) has long been recognized as a complication in people with chronic liver disease, particularly those with cirrhosis. Two gene therapies for haemophilia A and B recently approved in Europe and the US utilize adeno-associated virus (AAV) vectors designed to target hepatocytes. A number of other AAV gene therapies are undergoing clinical investigation for both liver and extrahepatic diseases, many of which likely transduce hepatocytes as well. Although AAV vectors predominantly persist in episomal forms, concerns about insertional mutagenesis have arisen due to findings in pre-clinical models and in a small subset of human HCC cases featuring wild-type AAV integrations in proximity to potential oncogenes. Despite the absence of any causative link between AAV vector therapy and HCC in approved extrahepatic gene therapies or haemophilia gene therapy trials, the package inserts for the recently approved haemophilia gene therapies advise HCC screening in subsets of individuals with additional risk factors. In this review, we discuss HCC risk factors, compare various screening modalities, discuss optimal screening intervals, and consider when to initiate and possibly discontinue screening. At this early point in the evolution of gene therapy, we lack sufficient data to make evidence-based recommendations on HCC screening. While AAV vectors may eventually be shown to be unassociated with risk of HCC, we presently favour a cautious approach that entails regular surveillance until such time as it is hopefully proven to be unnecessary.

基因治疗后的肝癌监测--多长时间监测一次?
长期以来,肝细胞癌(HCC)一直被认为是慢性肝病患者,尤其是肝硬化患者的一种并发症。欧洲和美国最近批准了两种治疗血友病 A 和 B 的基因疗法,它们使用的腺相关病毒(AAV)载体设计用于靶向肝细胞。目前正在对许多其他 AAV 基因疗法进行临床研究,以治疗肝病和肝外疾病,其中许多疗法也可能转导肝细胞。尽管AAV载体主要以外显子形式存在,但由于临床前模型和一小部分人类HCC病例中发现野生型AAV整合在潜在癌基因附近,人们对插入突变产生了担忧。尽管在已获批的肝外基因疗法或血友病基因疗法试验中,AAV载体疗法与HCC之间没有任何因果关系,但最近获批的血友病基因疗法的说明书建议对具有额外风险因素的人群进行HCC筛查。在这篇综述中,我们讨论了 HCC 风险因素,比较了各种筛查模式,讨论了最佳筛查时间间隔,并考虑了何时启动和可能中止筛查。在基因治疗发展的早期阶段,我们缺乏足够的数据就 HCC 筛查提出循证建议。虽然 AAV 向量最终可能会被证明与 HCC 风险无关,但我们目前倾向于采取一种谨慎的方法,即定期进行监测,直到有望证明没有必要为止。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Viral Hepatitis
Journal of Viral Hepatitis 医学-病毒学
CiteScore
6.00
自引率
8.00%
发文量
138
审稿时长
1.5 months
期刊介绍: The Journal of Viral Hepatitis publishes reviews, original work (full papers) and short, rapid communications in the area of viral hepatitis. It solicits these articles from epidemiologists, clinicians, pathologists, virologists and specialists in transfusion medicine working in the field, thereby bringing together in a single journal the important issues in this expanding speciality. The Journal of Viral Hepatitis is a monthly journal, publishing reviews, original work (full papers) and short rapid communications in the area of viral hepatitis. It brings together in a single journal important issues in this rapidly expanding speciality including articles from: virologists; epidemiologists; clinicians; pathologists; specialists in transfusion medicine.
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