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Genomic-scale comparison of sequence- and structure-based methods of function prediction: does structure provide additional insight?

机译:基于序列和基于结构的功能预测方法的基因组规模比较:结构是否提供其他见解?

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A function annotation method using the sequence-to-structure-to-function paradigm is applied to the identification of all disulfide oxidoreductases in the Saccharomyces cerevisiae genome. The method identifies 27 sequences as potential disulfide oxidoreductases. All previously known thioredoxins, glutaredoxins, and disulfide isomerases are correctly identified. Three of the 27 predictions are probable false-positives. Three novel predictions, which subsequently have been experimentally validated, are presented. Two additional novel predictions suggest a disulfide oxidoreductase regulatory mechanism for two subunits (OST3 and OST6) of the yeast oligosaccharyltransferase complex. Based on homology, this prediction can be extended to a potential tumor suppressor gene, N33, in humans, whose biochemical function was not previously known. Attempts to obtain a folded, active N33 construct to test the prediction were unsuccessful. The results show that structure prediction coupled with biochemically relevant structural motifs is a powerful method for the function annotation of genome sequences and can provide more detailed, robust predictions than function prediction methods that rely on sequence comparison alone.
机译:一种使用序列到结构到功能范式的功能注释方法,被用于啤酒酵母基因组中所有二硫键氧化还原酶的鉴定。该方法将27个序列鉴定为潜在的二硫键氧化还原酶。所有先前已知的硫氧还蛋白,戊二醛毒素和二硫键异构酶均已正确鉴定。 27个预测中的三个是可能的假阳性。提出了三种新颖的预测,随后进行了实验验证。另外两个新颖的预测表明,酵母寡糖基转移酶复合物的两个亚基(OST3和OST6)具有二硫化物氧化还原酶调节机制。基于同源性,该预测可以扩展至人类潜在的抑癌基因N33,其生化功能尚不清楚。尝试获得折叠的活性N33构建体以测试预测未成功。结果表明,结合生物化学相关结构基序的结构预测是一种功能强大的方法,可对基因组序列进行功能注释,比仅依赖序列比较的功能预测方法可提供更详细,更可靠的预测。

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