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Mapping the yeast host cell response to recombinant membrane protein production:relieving the biological bottlenecks

机译:绘制酵母宿主细胞对重组膜蛋白生产的反应图:缓解生物学瓶颈

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摘要

Understanding the structures and functions of membrane proteins is an active area of research within bioscience. Membrane proteins are key players in essential cellular processes such as the uptake of nutrients, the export of waste products, and the way in which cells communicate with their environment. It is therefore not surprising that membrane proteins are targeted by over half of all prescription drugs. Since most membrane proteins are not abundant in their native membranes, it is necessary to produce them in recombinant host cells to enable further structural and functional studies. Unfortunately, achieving the required yields of functional recombinant membrane proteins is still a bottleneck in contemporary bioscience. This has highlighted the need for defined and rational optimization strategies based upon experimental observation rather than relying on trial and error. We have published a transcriptome and subsequent genetic analysis that has identified genes implicated in high-yielding yeast cells. These results have highlighted a role for alterations to a cell's protein synthetic capacity in the production of high yields of recombinant membrane protein: paradoxically, reduced protein synthesis favors higher yields. These results highlight a potential bottleneck at the protein folding or translocation stage of protein production.
机译:了解膜蛋白的结构和功能是生物科学领域的活跃研究领域。膜蛋白是必需细胞过程中的关键角色,这些过程包括营养的吸收,废物的输出以及细胞与周围环境的通讯方式。因此不足为奇的是,所有处方药中超过一半都靶向膜蛋白。由于大多数膜蛋白在其天然膜中并不丰富,因此有必要在重组宿主细胞中生产它们,以进行进一步的结构和功能研究。不幸的是,实现所需的功能性重组膜蛋白产量仍然是当代生物科学的瓶颈。这突出了需要基于实验观察而不是依靠反复试验而确定和合理的优化策略。我们已经发表了一个转录组和随后的遗传分析,已经鉴定出与高产酵母细胞有关的基因。这些结果凸显了改变细胞蛋白质合成能力在高产量重组膜蛋白生产中的作用:矛盾的是,蛋白质合成减少有利于更高产量。这些结果突出了蛋白质生产中蛋白质折叠或易位阶段的潜在瓶颈。

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