A systematic review investigating advances in gene therapy for Fanconi anemia over the last three decades

Lorna M. McLeman, A. Glaser, R. Conyers, A. Deans
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Abstract

Fanconi anemia (FA) is the most common inherited bone marrow failure syndrome, characterized by cellular DNA repair deficiency, developmental defects, and a 700-fold increased risk of developing cancer. A bone marrow transplant is the only treatment option for the hematological manifestations of FA, but it can have serious complications. Gene therapy, on the other hand, offers a promising alternative, using cells from the patient that have been corrected ex vivo. However, due to the complexity of cells with a compromised DNA repair pathway, it has been difficult to achieve success in treating FA with gene therapy, despite advancements in the treatment of other blood disorders. This review summarizes all published human trials to date, including a recent study that reported success in treating four pediatric patients with gene therapy, and its interim Phase II study that has successfully treated six further patients. We discuss the key advances, such as improvements in viral vectors, shorter ex vivo transduction protocols, and the use of hypoxia and/or media additives such as N-acetylcysteine or etanercept. We also discuss the potential use of mobilizing agents such as granulocyte-colony stimulating factor (G-CSF) and plerixafor. The data from human trials are systematically reviewed and advances in murine and in vitro studies are discussed.
系统回顾了过去三十年来范可尼贫血基因治疗的进展
范可尼贫血(FA)是最常见的遗传性骨髓衰竭综合征,其特征是细胞DNA修复缺陷、发育缺陷和患癌症的风险增加700倍。骨髓移植是FA血液学表现的唯一治疗选择,但它可能有严重的并发症。另一方面,基因治疗提供了一种很有希望的替代方案,它使用的是患者体内经过体外校正的细胞。然而,由于DNA修复途径受损的细胞的复杂性,尽管在治疗其他血液疾病方面取得了进展,但用基因疗法治疗FA很难取得成功。本综述总结了迄今为止所有已发表的人体试验,包括最近一项研究,该研究报告成功地治疗了四名儿科患者的基因治疗,以及它的中期II期研究,该研究成功地治疗了另外六名患者。我们讨论了关键的进展,如病毒载体的改进,更短的体外转导方案,使用缺氧和/或培养基添加剂,如n -乙酰半胱氨酸或依那西普。我们还讨论了动员剂的潜在用途,如粒细胞集落刺激因子(G-CSF)和plerixafor。系统地回顾了人体试验的数据,并讨论了小鼠和体外研究的进展。
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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