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Concepts and tools to exploit the potential of bacterial inclusion bodies in protein science and biotechnology

机译:利用蛋白质科学和生物技术中细菌包涵体潜力的概念和工具

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摘要

Cells have evolved complex and overlapping mechanisms to protect their proteins from aggregation. However, several reasons can cause the failure of such defences, among them mutations, stress conditions and high rates of protein synthesis, all common consequences of heterologous protein production. As a result, in the bacterial cytoplasm several recombinant proteins aggregate as insoluble inclusion bodies. The recent discovery that aggregated proteins can retain native-like conformation and biological activity has opened the way for a dramatic change in the means by which intracellular aggregation is approached and exploited. This paper summarizes recent studies towards the direct use of inclusion bodies in biotechnology and for the detection of bottlenecks in the folding pathways of specific proteins. We also review the major biophysical methods available for revealing fine structural details of aggregated proteins and which information can be obtained through these techniques.
机译:细胞已经进化出复杂且重叠的机制来保护其蛋白质免于聚集。但是,有几种原因会导致这种防御的失败,其中包括突变,应激条件和高蛋白合成率,这都是异源蛋白生产的所有常见后果。结果,在细菌细胞质中,几种重组蛋白聚集为不溶性包涵体。聚集蛋白可以保留天然样构象和生物学活性的最新发现为细胞内聚集的接近和利用方式的巨大变化开辟了道路。本文概述了直接在生物技术中使用包涵体以及检测特定蛋白质折叠途径中瓶颈的最新研究。我们还回顾了可用于揭示聚集蛋白精细结构细节以及可通过这些技术获得哪些信息的主要生物物理方法。

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