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GTOP: a database of protein structures predicted from genome sequences

机译:GTOP:从基因组序列预测的蛋白质结构的数据库

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摘要

Large-scale genome projects generate an unprecedented number of protein sequences, most of them are experimentally uncharacterized. Predicting the 3D structures of sequences provides important clues as to their functions. We constructed the Genomes TO Protein structures and functions (GTOP) database, containing protein fold predictions of a huge number of sequences. Predictions are mainly carried out with the homology search program PSI-BLAST, currently the most popular among high-sensitivity profile search methods. GTOP also includes the results of other analyses, e.g. homology and motif search, detection of transmembrane helices and repetitive sequences. We have completed analyzing the sequences of 41 organisms, with the number of proteins exceeding 120 000 in total. GTOP uses a graphical viewer to present the analytical results of each ORF in one page in a ‘color-bar' format. The assigned 3D structures are presented by Chime plug-in or RasMol. The binding sites of ligands are also included, providing functional information. The GTOP server is available at http://spock.genes.nig.ac.jp/~genome/gtop.html.
机译:大规模的基因组计划会产生空前数量的蛋白质序列,其中大多数在实验上都不具有特征。预测序列的3D结构可提供有关其功能的重要线索。我们构建了Genomes TO蛋白质结构和功能(GTOP)数据库,其中包含大量序列的蛋白质折叠预测。预测主要通过同源性搜索程序PSI-BLAST进行,PSI-BLAST是目前在高灵敏度概图搜索方法中最流行的程序。 GTOP还包括其他分析的结果,例如同源性和基序搜索,跨膜螺旋和重复序列的检测。我们已经完成了41种生物的序列分析,蛋白质总数超过12万。 GTOP使用图形查看器以“颜色栏”格式在一页中显示每个ORF的分析结果。分配的3D结构由Chime插件或RasMol呈现。还包括配体的结合位点,提供功能信息。可从http://spock.genes.nig.ac.jp/~genome/gtop.html获得GTOP服务器。

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