Protein tertiary structure prediction is an active research area and has attracted significant attention recently due to the success of AlphaFold from DeepMind. Methods capable of accurately evaluating the quality of predicted models are of great importance. In the past, although many model quality assessment (QA) methods have been developed, their accuracies are not consistently high across different QA performance metrics for diverse target proteins. In this paper, we propose MUfoldQA_G, a new multi-model QA method that aims at simultaneously optimizing Pearson correlation and average GDT-TS difference, two commonly used QA performance metrics. This method is based on two new algorithms MUfoldQA_Gp and MUfoldQA_Gr. MUfoldQA_Gp uses a new technique to combine information from protein templates and reference protein models to maximize the Pearson correlation QA metric. MUfoldQA_Gr employs a new machine learning technique that resamples training data and retrains adaptively to learn a consensus model that is better than naïve consensus while minimizing average GDT-TS difference. MUfoldQA_G uses a new method to combine the results of MUfoldQA_Gr and MUfoldQA_Gp so that the final QA prediction results achieve low average GDT-TS difference that is close to the results from MUfoldQA_Gr, while maintaining high Pearson correlation that is the same as the results from MUfoldQA_Gp. In CASP14 QA categories, MUfoldQA_G ranked No. 1 in Pearson correlation and No. 2 in average GDT-TS difference.
Keywords: Multi-model QA methods; Protein model quality assessment; Protein structure prediction.
© 2021 The Author(s).