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Progress and prospects of engineered sequence-specific DNA modulating technologies for the management of liver diseases

机译:工程序列特异性DNA调控技术在肝病治疗中的研究进展与展望

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摘要

Liver diseases are one of the leading causes of mortality in the world. The hepatic illnesses, which include inherited metabolic disorders, hemophilias and viral hepatitides, are complex and currently difficult to treat. The maturation of gene therapy has heralded new avenues for developing effective intervention for these diseases. DNA modification using gene therapy is now possible and available technology may be exploited to achieve long term therapeutic benefit. The ability to edit DNA sequences specifically is of paramount importance to advance gene therapy for application to liver diseases. Recent development of technologies that allow for this has resulted in rapid advancement of gene therapy to treat several chronic illnesses. Improvements in application of derivatives of zinc finger proteins (ZFPs), transcription activator-like effectors (TALEs), homing endonucleases (HEs) and clustered regularly interspaced palindromic repeats (CRISPR) and CRISPR associated (Cas) systems have been particularly important. These sequence-specific technologies may be used to modify genes permanently and also to alter gene transcription for therapeutic purposes. This review describes progress in development of ZFPs, TALEs, HEs and CRISPR/Cas for application to treating liver diseases.
机译:肝病是世界上导致死亡的主要原因之一。包括遗传性代谢疾病,血友病和病毒性肝炎在内的肝病很复杂,目前很难治疗。基因治疗的成熟为开发针对这些疾病的有效干预手段开辟了新途径。现在可以使用基因疗法进行DNA修饰,并且可以利用可用的技术来获得长期的治疗益处。专门编辑DNA序列的能力对于推进应用于肝病的基因治疗至关重要。允许这种情况的技术的最新发展导致了用于治疗几种慢性疾病的基因治疗的迅速发展。锌指蛋白衍生物(ZFP),转录激活因子样效应物(TALE),归巢内切核酸酶(HE)以及簇状规则间隔回文重复序列(CRISPR)和CRISPR相关(Cas)系统的应用特别重要。这些序列特异性技术可用于永久修饰基因,也可用于治疗目的改变基因转录。这篇综述描述了用于治疗肝脏疾病的ZFP,TALE,HE和CRISPR / Cas的开发进展。

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