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首页> 外文期刊>ACS Chemical Biology >Yeast Tripartite Biosensors Sensitive to Protein Stability and Aggregation Propensity
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Yeast Tripartite Biosensors Sensitive to Protein Stability and Aggregation Propensity

机译:酵母三方生物传感器对蛋白质稳定性和聚集倾向敏感

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In contrast to the myriad approaches available to study protein misfolding and aggregation in vitro, relatively few tools are available for the study of these processes in the cellular context. This is in part due to the complexity of the cellular environment which, for instance, interferes with many spectroscopic approaches. Here, we describe a tripartite fusion approach that can be used to assess in vivo protein stability and solubility in the cytosol of Saccharomyces cerevisiae. Our biosensors contain tripartite fusions in which a protein of interest is inserted into antibiotic resistance markers. These fusions act to directly link the aggregation susceptibility and stability of the inserted protein to antibiotic resistance. We demonstrate a linear relationship between the thermodynamic stabilities of variants of the model folding protein immunity protein 7 (Im7) fused into the resistance markers and their antibiotic resistance readouts. We also use this system to investigate the in vivo properties of the yeast prion proteins Sup35 and Rnq1 and proteins whose aggregation is associated with some of the most prevalent neurodegenerative misfolding disorders, including peptide amyloid beta 1-42 (A beta 42), which is involved in Alzheimer's disease, and protein alpha-synuclein, which is linked to Parkinson's disease.
机译:与在体外学习蛋白质错误折叠和聚集的无数方法相比,在细胞背景下的这些过程可以获得相对较少的工具。这部分是由于蜂窝环境的复杂性,例如,这种复杂性地干扰了许多光谱方法。在这里,我们描述了一种三方融合方法,可用于评估酿酒酵母酿酒酵母细胞溶胶中的体内蛋白质稳定性和溶解度。我们的生物传感器包含三方融合,其中将感兴趣的蛋白质插入抗生素抗性标志物中。这些融合是直接将插入蛋白的聚集敏感性和稳定性联系到抗生素抗性。我们证明了模型折叠蛋白免疫蛋白7(IM7)的变体的热力稳定性之间的线性关系,融合到抗性标记物中及其抗生素抗性读出。我们还使用该系统来研究酵母朊病毒蛋白质Sup35和RNQ1的体内性质,并且其聚集与一些最普遍的神经退行性错误折叠紊乱有关的蛋白质,包括肽淀粉样蛋白β1-42(β22)参与阿尔茨海默病,蛋白质α-突触核蛋白,与帕金森病联系起来。

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