DOCKING-CALCULATION-BASED METHOD FOR PREDICTING PROTEIN-RNA INTERACTIONS
スポンサーリンク
概要
- 論文の詳細を見る
Elucidating protein-RNA interactions (PRIs) is important for understanding many cellular systems. We developed a PRI prediction method by using a rigid-body protein-RNA docking calculation with tertiary structure data. We evaluated this method by using 78 protein-RNA complex structures from the Protein Data Bank. We predicted the interactions for pairs in 78×78 combinations. Of these, 78 original complexes were defined as positive pairs, and the other 6,006 complexes were defined as negative pairs; then an F-measure value of 0.465 was obtained with our prediction system.
- 日本バイオインフォマティクス学会の論文
日本バイオインフォマティクス学会 | 論文
- Performance Improvement in Protein N-Myristoyl Classification by BONSAI with Insignificant Indexing Symbol
- A combined pathway to simulate CDK-dependent phosphorylation and ARF-dependent stabilization for p53 transcriptional activity
- A versatile petri net based architecture for modeling and simulation of complex biological processes
- XML documentation of biopathways and their simulations in Genomic Object Net
- Prediction of debacle points for robustness of biological pathways by using recurrent neural networks