医药用质粒DNA的生产。

Carsten Voss
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引用次数: 26

摘要

在基因层面上治疗疾病的概念早在20世纪70年代就已经提出,但在过去的16年里,只有分子生物学和基因操作工具的发展,才将这一概念带入实验室和诊所。病毒和非病毒载体和传递系统被开发用于将治疗基因转移到靶细胞中。在非病毒途径的情况下,质粒DNA已经成为一种非常有前途的基因传递载体,因为它可以很容易地通过培养含有大肠杆菌的质粒和随后的下游加工来进行基因操作和生产,因此与其他基因传递载体相比,它的生产更容易。使用质粒DNA的另一个优点是使用病毒载体时可能出现的免疫原性反应和癌原激活的风险较低。本文综述了质粒制造的最新进展,从细菌分批培养和补料分批培养到生产携带质粒的大肠杆菌,再到细胞裂解和随后的纯化,再到储存、应用、工艺和质量控制。
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Production of plasmid DNA for pharmaceutical use.

The concept of curing diseases at the genetic level was already introduced in the 1970s, but only the evolution of molecular biology and tools for genetic manipulation brought the idea into labs and clinics during the last 16 years. Viral and non-viral vectors and delivery systems were developed to transfer therapeutic genes into the target cells. In the case of non-viral approaches plasmid DNA has become a very promising gene delivery vector because it can easily be genetically manipulated and produced by cultivation of plasmid harbouring Escherichia coli and subsequent downstream processing, thus making production easy in comparison to other gene delivery vectors. Another advantage in using plasmid DNA is the low risk of immunogenic reactions and oncogen activation that can arise while using viral vectors. This review describes the recent development in plasmid manufacturing ranging from bacterial cultivation in batch and fedbatch mode to produce plasmid-bearing E. coli over cell lysis and subsequent purification to storage, application, and process and quality control.

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