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首页> 外文期刊>BMC Bioinformatics >SAMPLEX: Automatic mapping of perturbed and unperturbed regions of proteins and complexes
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SAMPLEX: Automatic mapping of perturbed and unperturbed regions of proteins and complexes

机译:SAMPLEX:自动绘制蛋白质和复合物的扰动和未扰动区域

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Background The activity of proteins within the cell is characterized by their motions, flexibility, interactions or even the particularly intriguing case of partially unfolded states. In the last two cases, a part of the protein is affected either by binding or unfolding and the detection of the respective perturbed and unperturbed region(s) is a fundamental part of the structural characterization of these states. This can be achieved by comparing experimental data of the same protein in two different states (bound/unbound, folded/unfolded). For instance, measurements of chemical shift perturbations (CSPs) from NMR 1H-15N HSQC experiments gives an excellent opportunity to discriminate both moieties. Results We describe an innovative, automatic and unbiased method to distinguish perturbed and unperturbed regions in a protein existing in two distinct states (folded/partially unfolded, bound/unbound). The SAMPLEX program takes as input a set of data and the corresponding three-dimensional structure and returns the confidence for each residue to be in a perturbed or unperturbed state. Its performance is demonstrated for different applications including the prediction of disordered regions in partially unfolded proteins and of interacting regions in protein complexes. Conclusions The proposed approach is suitable for partially unfolded states of proteins, local perturbations due to small ligands and protein-protein interfaces. The method is not restricted to NMR data, but is generic and can be applied to a wide variety of information.
机译:背景技术细胞内蛋白质的活性以其运动,柔韧性,相互作用或什至是部分展开状态的特别有趣的情况为特征。在最后两种情况下,蛋白质的一部分受到结合或解折叠的影响,检测到各自的扰动和未扰动区域是这些状态结构表征的基本部分。这可以通过比较处于两种不同状态(结合/未结合,折叠/未折叠)的相同蛋白质的实验数据来实现。例如,通过NMR 1 H- 15 N HSQC实验对化学位移扰动(CSP)的测量为区分这两个部分提供了极好的机会。结果我们描述了一种创新的,自动的和无偏见的方法来区分存在于两种不同状态(折叠/部分展开,结合/未结合)的蛋白质中的干扰和非干扰区域。 SAMPLEX程序将一组数据和相应的三维结构作为输入,并返回处于扰动或未扰动状态的每个残基的置信度。已证明其性能可用于各种应用,包括预测部分未折叠蛋白的无序区域和蛋白复合物的相互作用区域。结论所提出的方法适用于蛋白质的部分展开状态,由于小配体和蛋白质-蛋白质界面而引起的局部扰动。该方法不限于NMR数据,而是通用的,可以应用于多种信息。

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