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1. High‐throughput prediction of disordered moonlighting regions in protein sequences

   https://doi.org/10.1002/prot.25590  

   Meng, Fanchi ; Kurgan, Lukasz ( September 2018 , Proteins: Structure, Function, and Bioinformatics)

   Intrinsically disordered regions lack stable structure in their native conformation but are nevertheless functional and highly abundant, particularly in Eukaryotes. Disordered moonlighting regions (DMRs) are intrinsically disordered regions that carry out multiple functions. DMRs are different from moonlighting proteins that could be structured and that are annotated at the whole‐protein level. DMRs cannot be identified by current predictors of functions of disorder that focus on specific functions rather than multifunctional regions. We conceptualized, designed and empirically assessed first‐of‐its‐kind sequence‐based predictor of DMRs, DMRpred. This computational tool outputs propensity for being in a DMR for each residue in an input protein sequence. We developed novel amino acid indices that quantify propensities for functions relevant to DMRs and used evolutionary conservation, putative solvent accessibility and intrinsic disorder derived from the input sequence to build a rich profile that is suitable to accurately predict DMRs. We processed this profile to derive innovative features that we input into a Random Forest model to generate the predictions. Empirical assessment shows that DMRpred generates accurate predictions with area under receiver operating characteristic curve = 0.86 and accuracy = 82%. These results are significantly better than the closest alternative approaches that rely on sequence alignment, evolutionary conservation and putative disorder and disorder functions. Analysis of abundance of putative DMRs in the human proteome reveals that as many as 25% of proteins may have long >30 residues) DMRs. A webserver implementation of DMRpred is available athttp://biomine.cs.vcu.edu/servers/DMRpred/

    

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2. DISOselect: Disorder predictor selection at the protein level

   https://doi.org/10.1002/pro.3756  

   Katuwawala, Akila ; Oldfield, Christopher J. ; Kurgan, Lukasz ( November 2019 , Protein Science)

   The intense interest in the intrinsically disordered proteins in the life science community, together with the remarkable advancements in predictive technologies, have given rise to the development of a large number of computational predictors of intrinsic disorder from protein sequence. While the growing number of predictors is a positive trend, we have observed a considerable difference in predictive quality among predictors for individual proteins. Furthermore, variable predictor performance is often inconsistent between predictors for different proteins, and the predictor that shows the best predictive performance depends on the unique properties of each protein sequence. We propose a computational approach, DISOselect, to estimate the predictive performance of 12 selected predictors for individual proteins based on their unique sequence‐derived properties. This estimation informs the users about the expected predictive quality for a selected disorder predictor and can be used to recommend methods that are likely to provide the best quality predictions. Our solution does not depend on the results of any disorder predictor; the estimations are made based solely on the protein sequence. Our solution significantly improves predictive performance, as judged with a test set of 1,000 proteins, when compared to other alternatives. We have empirically shown that by using the recommended methods the overall predictive performance for a given set of proteins can be improved by a statistically significant margin. DISOselect is freely available for non‐commercial users through the webserver athttp://biomine.cs.vcu.edu/servers/DISOselect/.

    

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3. DEPICTER2: a comprehensive webserver for intrinsic disorder and disorder function prediction

   https://doi.org/10.1093/nar/gkad330  

   Basu, Sushmita ; Gsponer, Jörg ; Kurgan, Lukasz ( May 2023 , Nucleic Acids Research)

   Intrinsic disorder in proteins is relatively abundant in nature and essential for a broad spectrum of cellular functions. While disorder can be accurately predicted from protein sequences, as it was empirically demonstrated in recent community-organized assessments, it is rather challenging to collect and compile a comprehensive prediction that covers multiple disorder functions. To this end, we introduce the DEPICTER2 (DisorderEd PredictIon CenTER) webserver that offers convenient access to a curated collection of fast and accurate disorder and disorder function predictors. This server includes a state-of-the-art disorder predictor, flDPnn, and five modern methods that cover all currently predictable disorder functions: disordered linkers and protein, peptide, DNA, RNA and lipid binding. DEPICTER2 allows selection of any combination of the six methods, batch predictions of up to 25 proteins per request and provides interactive visualization of the resulting predictions. The webserver is freely available at http://biomine.cs.vcu.edu/servers/DEPICTER2/

    

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4. HybridDBRpred: improved sequence-based prediction of DNA-binding amino acids using annotations from structured complexes and disordered proteins

   https://doi.org/10.1093/nar/gkad1131  

   Zhang, Jian ; Basu, Sushmita ; Kurgan, Lukasz ( December 2023 , Nucleic Acids Research)

   Current predictors of DNA-binding residues (DBRs) from protein sequences belong to two distinct groups, those trained on binding annotations extracted from structured protein-DNA complexes (structure-trained) vs. intrinsically disordered proteins (disorder-trained). We complete the first empirical analysis of predictive performance across the structure- and disorder-annotated proteins for a representative collection of ten predictors. Majority of the structure-trained tools perform well on the structure-annotated proteins while doing relatively poorly on the disorder-annotated proteins, and vice versa. Several methods make accurate predictions for the structure-annotated proteins or the disorder-annotated proteins, but none performs highly accurately for both annotation types. Moreover, most predictors make excessive cross-predictions for the disorder-annotated proteins, where residues that interact with non-DNA ligand types are predicted as DBRs. Motivated by these results, we design, validate and deploy an innovative meta-model, hybridDBRpred, that uses deep transformer network to combine predictions generated by three best current predictors. HybridDBRpred provides accurate predictions and low levels of cross-predictions across the two annotation types, and is statistically more accurate than each of the ten tools and baseline meta-predictors that rely on averaging and logistic regression. We deploy hybridDBRpred as a convenient web server at http://biomine.cs.vcu.edu/servers/hybridDBRpred/ and provide the corresponding source code at https://github.com/jianzhang-xynu/hybridDBRpred.

    

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5. DescribePROT: database of amino acid-level protein structure and function predictions

   https://doi.org/10.1093/nar/gkaa931  

   Zhao, Bi ; Katuwawala, Akila ; Oldfield, Christopher J ; Dunker, A Keith ; Faraggi, Eshel ; Gsponer, Jörg ; Kloczkowski, Andrzej ; Malhis, Nawar ; Mirdita, Milot ; Obradovic, Zoran ; et al ( October 2020 , Nucleic Acids Research)

   null (Ed.)

   Abstract We present DescribePROT, the database of predicted amino acid-level descriptors of structure and function of proteins. DescribePROT delivers a comprehensive collection of 13 complementary descriptors predicted using 10 popular and accurate algorithms for 83 complete proteomes that cover key model organisms. The current version includes 7.8 billion predictions for close to 600 million amino acids in 1.4 million proteins. The descriptors encompass sequence conservation, position specific scoring matrix, secondary structure, solvent accessibility, intrinsic disorder, disordered linkers, signal peptides, MoRFs and interactions with proteins, DNA and RNAs. Users can search DescribePROT by the amino acid sequence and the UniProt accession number and entry name. The pre-computed results are made available instantaneously. The predictions can be accesses via an interactive graphical interface that allows simultaneous analysis of multiple descriptors and can be also downloaded in structured formats at the protein, proteome and whole database scale. The putative annotations included by DescriPROT are useful for a broad range of studies, including: investigations of protein function, applied projects focusing on therapeutics and diseases, and in the development of predictors for other protein sequence descriptors. Future releases will expand the coverage of DescribePROT. DescribePROT can be accessed at http://biomine.cs.vcu.edu/servers/DESCRIBEPROT/. 

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