511 research outputs found

    UFO: a web server for ultra-fast functional profiling of whole genome protein sequences

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    <p>Abstract</p> <p>Background</p> <p>Functional profiling is a key technique to characterize and compare the functional potential of entire genomes. The estimation of profiles according to an assignment of sequences to functional categories is a computationally expensive task because it requires the comparison of all protein sequences from a genome with a usually large database of annotated sequences or sequence families.</p> <p>Description</p> <p>Based on machine learning techniques for Pfam domain detection, the UFO web server for ultra-fast functional profiling allows researchers to process large protein sequence collections instantaneously. Besides the frequencies of Pfam and GO categories, the user also obtains the sequence specific assignments to Pfam domain families. In addition, a comparison with existing genomes provides dissimilarity scores with respect to 821 reference proteomes. Considering the underlying UFO domain detection, the results on 206 test genomes indicate a high sensitivity of the approach. In comparison with current state-of-the-art HMMs, the runtime measurements show a considerable speed up in the range of four orders of magnitude. For an average size prokaryotic genome, the computation of a functional profile together with its comparison typically requires about 10 seconds of processing time.</p> <p>Conclusion</p> <p>For the first time the UFO web server makes it possible to get a quick overview on the functional inventory of newly sequenced organisms. The genome scale comparison with a large number of precomputed profiles allows a first guess about functionally related organisms. The service is freely available and does not require user registration or specification of a valid email address.</p

    Modelling and recognition of protein contact networks by multiple kernel learning and dissimilarity representations

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    Multiple kernel learning is a paradigm which employs a properly constructed chain of kernel functions able to simultaneously analyse different data or different representations of the same data. In this paper, we propose an hybrid classification system based on a linear combination of multiple kernels defined over multiple dissimilarity spaces. The core of the training procedure is the joint optimisation of kernel weights and representatives selection in the dissimilarity spaces. This equips the system with a two-fold knowledge discovery phase: by analysing the weights, it is possible to check which representations are more suitable for solving the classification problem, whereas the pivotal patterns selected as representatives can give further insights on the modelled system, possibly with the help of field-experts. The proposed classification system is tested on real proteomic data in order to predict proteins' functional role starting from their folded structure: specifically, a set of eight representations are drawn from the graph-based protein folded description. The proposed multiple kernel-based system has also been benchmarked against a clustering-based classification system also able to exploit multiple dissimilarities simultaneously. Computational results show remarkable classification capabilities and the knowledge discovery analysis is in line with current biological knowledge, suggesting the reliability of the proposed system

    Integration and mining of malaria molecular, functional and pharmacological data: how far are we from a chemogenomic knowledge space?

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    The organization and mining of malaria genomic and post-genomic data is highly motivated by the necessity to predict and characterize new biological targets and new drugs. Biological targets are sought in a biological space designed from the genomic data from Plasmodium falciparum, but using also the millions of genomic data from other species. Drug candidates are sought in a chemical space containing the millions of small molecules stored in public and private chemolibraries. Data management should therefore be as reliable and versatile as possible. In this context, we examined five aspects of the organization and mining of malaria genomic and post-genomic data: 1) the comparison of protein sequences including compositionally atypical malaria sequences, 2) the high throughput reconstruction of molecular phylogenies, 3) the representation of biological processes particularly metabolic pathways, 4) the versatile methods to integrate genomic data, biological representations and functional profiling obtained from X-omic experiments after drug treatments and 5) the determination and prediction of protein structures and their molecular docking with drug candidate structures. Progresses toward a grid-enabled chemogenomic knowledge space are discussed.Comment: 43 pages, 4 figures, to appear in Malaria Journa

    Local protein structure prediction using discriminative models

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    BACKGROUND: In recent years protein structure prediction methods using local structure information have shown promising improvements. The quality of new fold predictions has risen significantly and in fold recognition incorporation of local structure predictions led to improvements in the accuracy of results. We developed a local structure prediction method to be integrated into either fold recognition or new fold prediction methods. For each local sequence window of a protein sequence the method predicts probability estimates for the sequence to attain particular local structures from a set of predefined local structure candidates. The first step is to define a set of local structure representatives based on clustering recurrent local structures. In the second step a discriminative model is trained to predict the local structure representative given local sequence information. RESULTS: The step of clustering local structures yields an average RMSD quantization error of 1.19 Å for 27 structural representatives (for a fragment length of 7 residues). In the prediction step the area under the ROC curve for detection of the 27 classes ranges from 0.68 to 0.88. CONCLUSION: The described method yields probability estimates for local protein structure candidates, giving signals for all kinds of local structure. These local structure predictions can be incorporated either into fold recognition algorithms to improve alignment quality and the overall prediction accuracy or into new fold prediction methods

    A comprehensive system for evaluation of remote sequence similarity detection

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    <p>Abstract</p> <p>Background</p> <p>Accurate and sensitive performance evaluation is crucial for both effective development of better structure prediction methods based on sequence similarity, and for the comparative analysis of existing methods. Up to date, there has been no satisfactory comprehensive evaluation method that (i) is based on a large and statistically unbiased set of proteins with clearly defined relationships; and (ii) covers all performance aspects of sequence-based structure predictors, such as sensitivity and specificity, alignment accuracy and coverage, and structure template quality.</p> <p>Results</p> <p>With the aim of designing such a method, we (i) select a statistically balanced set of divergent protein domains from SCOP, and define similarity relationships for the majority of these domains by complementing the best of information available in SCOP with a rigorous SVM-based algorithm; and (ii) develop protocols for the assessment of similarity detection and alignment quality from several complementary perspectives. The evaluation of similarity detection is based on ROC-like curves and includes several complementary approaches to the definition of true/false positives. Reference-dependent approaches use the 'gold standard' of pre-defined domain relationships and structure-based alignments. Reference-independent approaches assess the quality of structural match predicted by the sequence alignment, with respect to the whole domain length (global mode) or to the aligned region only (local mode). Similarly, the evaluation of alignment quality includes several reference-dependent and -independent measures, in global and local modes. As an illustration, we use our benchmark to compare the performance of several methods for the detection of remote sequence similarities, and show that different aspects of evaluation reveal different properties of the evaluated methods, highlighting their advantages, weaknesses, and potential for further development.</p> <p>Conclusion</p> <p>The presented benchmark provides a new tool for a statistically unbiased assessment of methods for remote sequence similarity detection, from various complementary perspectives. This tool should be useful both for users choosing the best method for a given purpose, and for developers designing new, more powerful methods. The benchmark set, reference alignments, and evaluation codes can be downloaded from <url>ftp://iole.swmed.edu/pub/evaluation/</url>.</p

    Graph-based methods for large-scale protein classification and orthology inference

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    The quest for understanding how proteins evolve and function has been a prominent and costly human endeavor. With advances in genomics and use of bioinformatics tools, the diversity of proteins in present day genomes can now be studied more efficiently than ever before. This thesis describes computational methods suitable for large-scale protein classification of many proteomes of diverse species. Specifically, we focus on methods that combine unsupervised learning (clustering) techniques with the knowledge of molecular phylogenetics, particularly that of orthology. In chapter 1 we introduce the biological context of protein structure, function and evolution, review the state-of-the-art sequence-based protein classification methods, and then describe methods used to validate the predictions. Finally, we present the outline and objectives of this thesis. Evolutionary (phylogenetic) concepts are instrumental in studying subjects as diverse as the diversity of genomes, cellular networks, protein structures and functions, and functional genome annotation. In particular, the detection of orthologous proteins (genes) across genomes provides reliable means to infer biological functions and processes from one organism to another. Chapter 2 evaluates the available computational tools, such as algorithms and databases, used to infer orthologous relationships between genes from fully sequenced genomes. We discuss the main caveats of large-scale orthology detection in general as well as the merits and pitfalls of each method in particular. We argue that establishing true orthologous relationships requires a phylogenetic approach which combines both trees and graphs (networks), reliable species phylogeny, genomic data for more than two species, and an insight into the processes of molecular evolution. Also proposed is a set of guidelines to aid researchers in selecting the correct tool. Moreover, this review motivates further research in developing reliable and scalable methods for functional and phylogenetic classification of large protein collections. Chapter 3 proposes a framework in which various protein knowledge-bases are combined into unique network of mappings (links), and hence allows comparisons to be made between expert curated and fully-automated protein classifications from a single entry point. We developed an integrated annotation resource for protein orthology, ProGMap (Protein Group Mappings, http://www.bioinformatics.nl/progmap), to help researchers and database annotators who often need to assess the coherence of proposed annotations and/or group assignments, as well as users of high throughput methodologies (e.g., microarrays or proteomics) who deal with partially annotated genomic data. ProGMap is based on a non-redundant dataset of over 6.6 million protein sequences which is mapped to 240,000 protein group descriptions collected from UniProt, RefSeq, Ensembl, COG, KOG, OrthoMCL-DB, HomoloGene, TRIBES and PIRSF using a fast and fully automated sequence-based mapping approach. The ProGMap database is equipped with a web interface that enables queries to be made using synonymous sequence identifiers, gene symbols, protein functions, and amino acid or nucleotide sequences. It incorporates also services, namely BLAST similarity search and QuickMatch identity search, for finding sequences similar (or identical) to a query sequence, and tools for presenting the results in graphic form. Graphs (networks) have gained an increasing attention in contemporary biology because they have enabled complex biological systems and processes to be modeled and better understood. For example, protein similarity networks constructed of all-versus-all sequence comparisons are frequently used to delineate similarity groups, such as protein families or orthologous groups in comparative genomics studies. Chapter 4.1 presents a benchmark study of freely available graph software used for this purpose. Specifically, the computational complexity of the programs is investigated using both simulated and biological networks. We show that most available software is not suitable for large networks, such as those encountered in large-scale proteome analyzes, because of the high demands on computational resources. To address this, we developed a fast and memory-efficient graph software, netclust (http://www.bioinformatics.nl/netclust/), which can scale to large protein networks, such as those constructed of millions of proteins and sequence similarities, on a standard computer. An extended version of this program called Multi-netclust is presented in chapter 4.2. This tool that can find connected clusters of data presented by different network data sets. It uses user-defined threshold values to combine the data sets in such a way that clusters connected in all or in either of the networks can be retrieved efficiently. Automated protein sequence clustering is an important task in genome annotation projects and phylogenomic studies. During the past years, several protein clustering programs have been developed for delineating protein families or orthologous groups from large sequence collections. However, most of these programs have not been benchmarked systematically, in particular with respect to the trade-off between computational complexity and biological soundness. In chapter 5 we evaluate three best known algorithms on different protein similarity networks and validation (or 'gold' standard) data sets to find out which one can scale to hundreds of proteomes and still delineate high quality similarity groups at the minimum computational cost. For this, a reliable partition-based approach was used to assess the biological soundness of predicted groups using known protein functions, manually curated protein/domain families and orthologous groups available in expert-curated databases. Our benchmark results support the view that a simple and computationally cheap method such as netclust can perform similar to and in cases even better than more sophisticated, yet much more costly methods. Moreover, we introduce an efficient graph-based method that can delineate protein orthologs of hundreds of proteomes into hierarchical similarity groups de novo. The validity of this method is demonstrated on data obtained from 347 prokaryotic proteomes. The resulting hierarchical protein classification is not only in agreement with manually curated classifications but also provides an enriched framework in which the functional and evolutionary relationships between proteins can be studied at various levels of specificity. Finally, in chapter 6 we summarize the main findings and discuss the merits and shortcomings of the methods developed herein. We also propose directions for future research. The ever increasing flood of new sequence data makes it clear that we need improved tools to be able to handle and extract relevant (orthological) information from these protein data. This thesis summarizes these needs and how they can be addressed by the available tools, or be improved by the new tools that were developed in the course of this research. <br/

    LFM-Pro: a tool for detecting significant local structural sites in proteins

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    Motivation: The rapidly growing protein structure repositories have opened up new opportunities for discovery and analysis of functional and evolutionary relationships among proteins. Detecting conserved structural sites that are unique to a protein family is of great value in identification of functionally important atoms and residues. Currently available methods are computationally expensive and fail to detect biologically significant local features

    A Survey on Metric Learning for Feature Vectors and Structured Data

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    The need for appropriate ways to measure the distance or similarity between data is ubiquitous in machine learning, pattern recognition and data mining, but handcrafting such good metrics for specific problems is generally difficult. This has led to the emergence of metric learning, which aims at automatically learning a metric from data and has attracted a lot of interest in machine learning and related fields for the past ten years. This survey paper proposes a systematic review of the metric learning literature, highlighting the pros and cons of each approach. We pay particular attention to Mahalanobis distance metric learning, a well-studied and successful framework, but additionally present a wide range of methods that have recently emerged as powerful alternatives, including nonlinear metric learning, similarity learning and local metric learning. Recent trends and extensions, such as semi-supervised metric learning, metric learning for histogram data and the derivation of generalization guarantees, are also covered. Finally, this survey addresses metric learning for structured data, in particular edit distance learning, and attempts to give an overview of the remaining challenges in metric learning for the years to come.Comment: Technical report, 59 pages. Changes in v2: fixed typos and improved presentation. Changes in v3: fixed typos. Changes in v4: fixed typos and new method

    Automated Protein Subfamily Identification and Classification

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    Function prediction by homology is widely used to provide preliminary functional annotations for genes for which experimental evidence of function is unavailable or limited. This approach has been shown to be prone to systematic error, including percolation of annotation errors through sequence databases. Phylogenomic analysis avoids these errors in function prediction but has been difficult to automate for high-throughput application. To address this limitation, we present a computationally efficient pipeline for phylogenomic classification of proteins. This pipeline uses the SCI-PHY (Subfamily Classification in Phylogenomics) algorithm for automatic subfamily identification, followed by subfamily hidden Markov model (HMM) construction. A simple and computationally efficient scoring scheme using family and subfamily HMMs enables classification of novel sequences to protein families and subfamilies. Sequences representing entirely novel subfamilies are differentiated from those that can be classified to subfamilies in the input training set using logistic regression. Subfamily HMM parameters are estimated using an information-sharing protocol, enabling subfamilies containing even a single sequence to benefit from conservation patterns defining the family as a whole or in related subfamilies. SCI-PHY subfamilies correspond closely to functional subtypes defined by experts and to conserved clades found by phylogenetic analysis. Extensive comparisons of subfamily and family HMM performances show that subfamily HMMs dramatically improve the separation between homologous and non-homologous proteins in sequence database searches. Subfamily HMMs also provide extremely high specificity of classification and can be used to predict entirely novel subtypes. The SCI-PHY Web server at http://phylogenomics.berkeley.edu/SCI-PHY/ allows users to upload a multiple sequence alignment for subfamily identification and subfamily HMM construction. Biologists wishing to provide their own subfamily definitions can do so. Source code is available on the Web page. The Berkeley Phylogenomics Group PhyloFacts resource contains pre-calculated subfamily predictions and subfamily HMMs for more than 40,000 protein families and domains at http://phylogenomics.berkeley.edu/phylofacts/
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