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Relieving the first bottleneck in the drug discovery pipeline: using array technologies to rationalize membrane protein production.

机译:消除药物开发流程中的第一个瓶颈:使用阵列技术合理化膜蛋白的生产。

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摘要

The slow down in the drug discovery pipeline is, in part, owing to a lack of structural and functional information available for new drug targets. Membrane proteins, the targets of well over 50% of marketed pharmaceuticals, present a particular challenge. As they are not naturally abundant, they must be produced recombinantly for the structural biology that is a prerequisite to structure-based drug design. Unfortunately, however, obtaining high yields of functional, recombinant membrane proteins remains a major bottleneck in contemporary bioscience. While repeated rounds of trial-and-error optimization have not (and cannot) reveal mechanistic details of the biology of recombinant protein production, examination of the host response has provided new insights. To this end, we published an early transcriptome analysis that identified genes implicated in high-yielding yeast cell factories, which has enabled the engineering of improved production strains. These advances offer hope that the bottleneck of membrane protein production can be relieved rationally.
机译:药物发现流程的放缓部分是由于缺乏可用于新药物靶标的结构和功能信息。膜蛋白是市场上超过50%的药物的目标,这是一个特殊的挑战。由于它们不是天然丰富的,因此必须重组生产以用于基于结构药物设计的前提的结构生物学。然而,不幸的是,获得高产量的功能性重组膜蛋白仍然是当代生物科学的主要瓶颈。虽然反复的反复试验优化没有(也不能)揭示重组蛋白生产生物学的机制细节,但是对宿主反应的检查提供了新的见解。为此,我们发表了一项早期转录组分析,该分析鉴定了与高产酵母细胞工厂有关的基因,从而能够设计出改良的生产菌株。这些进展提供了希望,可以合理地缓解膜蛋白生产的瓶颈。

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