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首页> 外文期刊>Protein Science: A Publication of the Protein Society >Protein surface analysis for function annotation in high-throughput structural genomics pipeline.
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Protein surface analysis for function annotation in high-throughput structural genomics pipeline.

机译:用于高通量结构基因组学管道中功能注释的蛋白质表面分析。

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摘要

Structural genomics (SG) initiatives are expanding the universe of protein fold space by rapidly determining structures of proteins that were intentionally selected on the basis of low sequence similarity to proteins of known structure. Often these proteins have no associated biochemical or cellular functions. The SG success has resulted in an accelerated deposition of novel structures. In some cases the structural bioinformatics analysis applied to these novel structures has provided specific functional assignment. However, this approach has also uncovered limitations in the functional analysis of uncharacterized proteins using traditional sequence and backbone structure methodologies. A novel method, named pvSOAR (pocket and void Surface of Amino Acid Residues), of comparing the protein surfaces of geometrically defined pockets and voids was developed. pvSOAR was able to detect previously unrecognized and novel functional relationships between surface features of proteins. In this study, pvSOAR is applied to several structural genomics proteins. We examined the surfaces of YecM, BioH, and RpiB from Escherichia coli as well as the CBS domains from inosine-5'-monosphate dehydrogenase from Streptococcus pyogenes, conserved hypothetical protein Ta549 from Thermoplasm acidophilum, and CBS domain protein mt1622 from Methanobacterium thermoautotrophicum with the goal to infer information about their biochemical function.
机译:结构基因组学(SG)计划通过快速确定基于与已知结构的蛋白质的低序列相似性有意选择的蛋白质结构,扩展了蛋白质折叠空间的范围。这些蛋白质通常没有相关的生化或细胞功能。 SG的成功导致新型结构的加速沉积。在某些情况下,应用于这些新颖结构的结构生物信息学分析提供了特定的功能分配。但是,这种方法还发现了使用传统序列和主链结构方法对未表征蛋白质进行功能分析时的局限性。开发了一种新的方法,称为pvSOAR(氨基酸残基的空洞和空洞表面),用于比较几何定义的空洞和空洞的蛋白质表面。 pvSOAR能够检测蛋白质表面特征之间以前无法识别的新颖功能关系。在这项研究中,pvSOAR被应用于几种结构基因组蛋白。我们检查了大肠杆菌的YecM,BioH和RpiB的表面,以及化脓性链球菌的肌苷5'-单磷酸盐脱氢酶的CBS结构域,嗜酸嗜热菌的保守假设蛋白Ta549和甲基化嗜热甲烷化杆菌的CBS结构域蛋白mt1622与目的是推断有关其生化功能的信息。

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