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蛋白质结构简单比较模型中附加值的系统分析。

Systematic analysis of added-value in simple comparative models of protein structure.

作者信息

Chakravarty Suvobrata, Sanchez Roberto

机构信息

Structural Biology Program, Department of Physiology and Biophysics, Mount Sinai School of Medicine, New York, New York 10029, USA.

出版信息

Structure. 2004 Aug;12(8):1461-70. doi: 10.1016/j.str.2004.05.018.

Abstract

Added-value is the additional information that a model carries with respect to the template structure used for model building. Thousands of single-template models, corresponding to proteins of known structure, were analyzed. The accuracy of structure-derived properties, such as residue accessibility, surface area, electrostatic potential, and others, was determined as a function of template:target sequence identity by comparing the models with their corresponding experimental structures. Added-value was determined by comparing the accuracy in models with that from templates. Geometry-dependent properties such as neighborhood of buried residues and accessible surface area showed low added-value. Properties that also depend on the protein sequence, such as presence of polar areas and electrostatic potential, showed high added-value. In general added-value increases when template:target sequence identity decreases, but it is also affected by alignment errors. This study justifies the use of models instead of the use of templates to estimate structure-derived properties of a target protein.

摘要

附加值是模型相对于用于构建模型的模板结构所携带的额外信息。分析了数千个与已知结构蛋白质相对应的单模板模型。通过将模型与其相应的实验结构进行比较,确定了诸如残基可及性、表面积、静电势等结构衍生属性的准确性,作为模板与目标序列同一性的函数。通过比较模型与模板的准确性来确定附加值。诸如埋藏残基的邻域和可及表面积等几何相关属性显示出较低的附加值。也依赖于蛋白质序列的属性,如极性区域的存在和静电势,显示出较高的附加值。一般来说,当模板与目标序列同一性降低时,附加值会增加,但它也会受到比对错误的影响。这项研究证明了使用模型而非模板来估计目标蛋白质的结构衍生属性的合理性。

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