计算生物学
生物信息学
DNA
RNA结合蛋白
核糖核酸
蛋白质测序
生物
生物化学
肽序列
基因
作者
Jiajun Qiu,Michael Bernhofer,Michael Heinzinger,Sofie Kemper,Tomás Norambuena,Francisco Melo,Burkhard Rost
标识
DOI:10.1016/j.jmb.2020.02.026
摘要
The intricate details of how proteins bind to proteins, DNA, and RNA are crucial for the understanding of almost all biological processes. Disease-causing sequence variants often affect binding residues. Here, we described a new, comprehensive system of in silico methods that take only protein sequence as input to predict binding of protein to DNA, RNA, and other proteins. Firstly, we needed to develop several new methods to predict whether or not proteins bind (per-protein prediction). Secondly, we developed independent methods that predict which residues bind (per-residue). Not requiring three-dimensional information, the system can predict the actual binding residue. The system combined homology-based inference with machine learning and motif-based profile-kernel approaches with word-based (ProtVec) solutions to machine learning protein level predictions. This achieved an overall non-exclusive three-state accuracy of 77% ± 1% (±one standard error) corresponding to a 1.8 fold improvement over random (best classification for protein-protein with F1 = 91 ± 0.8%). Standard neural networks for per-residue binding residue predictions appeared best for DNA-binding (Q2 = 81 ± 0.9%) followed by RNA-binding (Q2 = 80 ± 1%) and worst for protein-protein binding (Q2 = 69 ± 0.8%). The new method, dubbed ProNA2020, is available as code through github (https://github.com/Rostlab/ProNA2020.git) and through PredictProtein (www.predictprotein.org).
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