Analysis of the Human Kinome Using Methods Including Fold Recognition Reveals Two Novel Kinases
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https://figshare.com/articles/dataset/Analysis_of_the_Human_Kinome_Using_Methods_Including_Fold_Recognition_Reveals_Two_Novel_Kinases/151036
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BackgroundProtein sequence similarity is a commonly used criterion for inferring the unknown function of a protein from a protein of known function. However, proteins can diverge significantly over time such that sequence similarity is difficult, if not impossible, to find. In some cases, a structural similarity remains over long evolutionary time scales and once detected can be used to predict function.
Methodology/Principal FindingsHere we employed a high-throughput approach to assign structural and functional annotation to the human proteome, focusing on the collection of human protein kinases, the human kinome. We compared human protein sequences to a library of domains from known structures using WU-BLAST, PSI-BLAST, and 123D. This approach utilized both sequence comparison and fold recognition methods. The resulting set of potential protein kinases was cross-checked against previously identified human protein kinases, and analyzed for conserved kinase motifs.
Conclusions/SignificanceWe demonstrate that our structure-based method can be used to identify both typical and atypical human protein kinases. We also identify two potentially novel kinases that contain an interesting combination of kinase and acyl-CoA dehydrogenase domains.
创建时间:
2008-02-13



