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PNAS Plus: Bacterial proteostasis balances energy and chaperone utilization efficiently

机译:PNAS Plus:细菌蛋白稳定平衡能量和分子伴侣的有效利用

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摘要

Chaperones are protein complexes that help to fold and disaggregate a cell’s proteins. It is not understood how four major chaperone systems of Escherichia coli work together in proteostasis: the recognition, sorting, folding, and disaggregating of the cell’s many different proteins. Here, we model this machine. We combine extensive data on chaperoning, folding, and aggregation rates with expression levels of proteins and chaperones measured at different growth rates. We find that the proteostasis machine recognizes and sorts a client protein based on two biophysical properties of the client’s misfolded state (M state): its stability and its kinetic accessibility from its unfolded state (U state). The machine is energy-efficient (the sickest proteins use the most ATP-expensive chaperones), comprehensive (it can handle any type of protein), and economical (the chaperone concentrations are just high enough to keep the whole proteome folded and disaggregated but no higher). The cell needs higher chaperone levels in two situations: fast growth (when protein production rates are high) and very slow growth (to mitigate the effects of protein degradation). This type of model complements experimental knowledge by showing how the various chaperones work together to achieve the broad folding and disaggregation needs of the cell.
机译:伴侣蛋白是一种蛋白质复合物,有助于折叠和分解细胞的蛋白质。目前尚不了解大肠杆菌的四个主要分子伴侣系统如何在蛋白质稳态中协同工作:细胞中许多不同蛋白质的识别,分类,折叠和分解。在这里,我们为这台机器建模。我们将有关伴侣,折叠和聚集速率的大量数据与以不同增长率测量的蛋白质和伴侣的表达水平结合在一起。我们发现蛋白质变形机器会根据客户错误折叠状态(M状态)的两个生物物理特性识别并分类客户蛋白质:其稳定性和从展开状态(U状态)的动力学可及性。该机器具有高能效(最病的蛋白质使用最昂贵的ATP分子伴侣),功能全面(可以处理任何类型的蛋白质)且经济(分子伴侣的浓度足够高,可以使整个蛋白质组折叠和分解,但没有)更高)。在两种情况下,细胞需要更高的伴侣水平:快速生长(蛋白质生产率高时)和非常缓慢的生长(以减轻蛋白质降解的影响)。这种类型的模型通过展示各种分子伴侣如何协同工作来实现细胞的广泛折叠和分解需求,从而补充了实验知识。

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