Add to ORKGQuantitative evaluation of binding affinity changes upon mutations is crucial for protein engineering and drug design. Machine learning-based methods are gaining increasing momentum in this field. Due to the limited number of experimental data, using a small number of sensitive predictive features is vital to the generalization and robustness of such machine learning methods. Here we introduce a fast and reliable predictor of binding affinity changes upon single point mutation, based on a random forest approach. Our method, iSEE, uses a limited number of interface Structure, Evolution and Energy-based features for the prediction. iSEE achieves, using only 31 features, a high prediction performance with a Pearson correlation coefficient (PCC...
Protein mutations, especially those which occur in the binding site, play an important role in inter...
Motivation Single protein residue mutations may reshape the binding affinity of protein¿protein int...
Statistics of the original data set, including the mutation type, the ID of the corresponding mutant...
Quantitative evaluation of binding affinity changes upon mutations is crucial for protein engineerin...
Quantitative evaluation of binding affinity changes upon mutations is crucial for protein engineerin...
<div><p>The formation of protein-protein complexes is essential for proteins to perform their physio...
Reliable prediction of binding affinity changes (ΔΔG) upon mutations in protein complexes relies not...
The aim of this thesis is to promote the understanding of protein-protein interactions (PPIs) by gai...
Predicting the structure and thermodynamics of protein–protein interactions (PPIs) are key to a prop...
Advances in sequencing have led to a rapid accumulation of mutations, some of which are associated w...
Protein-protein Interactions are involved in most fundamental biological processes, with disease cau...
Protein-protein Interactions are involved in most fundamental biological processes, with disease cau...
<div><p>Advances in sequencing have led to a rapid accumulation of mutations, some of which are asso...
The formation of protein-protein complexes is essential for proteins to perform their physio-logical...
Protein-protein interactions play a crucial role in all cellular functions and biological processes ...
Protein mutations, especially those which occur in the binding site, play an important role in inter...
Motivation Single protein residue mutations may reshape the binding affinity of protein¿protein int...
Statistics of the original data set, including the mutation type, the ID of the corresponding mutant...
Quantitative evaluation of binding affinity changes upon mutations is crucial for protein engineerin...
Quantitative evaluation of binding affinity changes upon mutations is crucial for protein engineerin...
<div><p>The formation of protein-protein complexes is essential for proteins to perform their physio...
Reliable prediction of binding affinity changes (ΔΔG) upon mutations in protein complexes relies not...
The aim of this thesis is to promote the understanding of protein-protein interactions (PPIs) by gai...
Predicting the structure and thermodynamics of protein–protein interactions (PPIs) are key to a prop...
Advances in sequencing have led to a rapid accumulation of mutations, some of which are associated w...
Protein-protein Interactions are involved in most fundamental biological processes, with disease cau...
Protein-protein Interactions are involved in most fundamental biological processes, with disease cau...
<div><p>Advances in sequencing have led to a rapid accumulation of mutations, some of which are asso...
The formation of protein-protein complexes is essential for proteins to perform their physio-logical...
Protein-protein interactions play a crucial role in all cellular functions and biological processes ...
Protein mutations, especially those which occur in the binding site, play an important role in inter...
Motivation Single protein residue mutations may reshape the binding affinity of protein¿protein int...
Statistics of the original data set, including the mutation type, the ID of the corresponding mutant...