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Large-Scale Analysis of Breast Cancer-Related Conformational Changes in Proteins Using Limited Proteolysis

机译:使用有限的蛋白水解大规模分析与乳腺癌相关的蛋白质构象变化

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摘要

Conformational changes in proteins can lead to disease. Thus, methods for identifying conformational changes in proteins can further improve our understanding and facilitate detection of disease states. Here we combine Culture (SILAC) to characterize breast cancer-related conformational changes in proteins on the proteomic scale. Studied here are the conformational properties of proteins in two cell culture models of breast cancer, including the MCF-10A and MCF-7 cell lines. The SILAC-LiP approach described here identified similar to 200 proteins with cell-line-dependent conformational changes, as determined by their differential susceptibility to proteolytic digestion using the nonspecific protease, proteinase K. The protease susceptibility profiles of the proteins in these cell lines were compared to thermodynamic stability and expression level profiles previously generated for proteins in these same breast cancer cell lines. The comparisons revealed that there was little overlap between the proteins with protease susceptibility changes and the proteins with thermodynamic stability and/or expression level changes. Thus, the large-scale conformational analysis described here provides unique insight into the molecular basis of the breast cancer phenotypes in this study.
机译:蛋白质的构象变化可能导致疾病。因此,鉴定蛋白质构象变化的方法可以进一步改善我们的理解并促进疾病状态的检测。在这里,我们结合文化(SILAC)来表征蛋白质组学上与乳腺癌相关的蛋白质构象变化。本文研究的是两种乳腺癌细胞培养模型中蛋白质的构象特性,包括MCF-10A和MCF-7细胞系。此处描述的SILAC-LiP方法鉴定出约200种具有细胞系依赖性构象变化的蛋白质,这取决于它们对使用非特异性蛋白酶K的蛋白水解消化的差异敏感性。这些蛋白质在这些细胞系中的蛋白酶敏感性谱为与先前在这些相同的乳腺癌细胞系中为蛋白质生成的热力学稳定性和表达水平概况进行比较。比较表明,具有蛋白酶敏感性变化的蛋白质与具有热力学稳定性和/或表达水平变化的蛋白质之间几乎没有重叠。因此,在此描述的大规模构象分析提供了对乳腺癌表型分子基础的独特见解。

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