Large-scale Characterization of Intrinsic Disorder and High-throughput Prediction Of RNA, DNA and Protein Binding Mediated by Intrinsic Disorder

Large-scale Characterization of Intrinsic Disorder and High-throughput Prediction Of RNA, DNA and Protein Binding Mediated by Intrinsic Disorder PDF Author: Zhenling Peng
Publisher:
ISBN:
Category : Bioinformatics
Languages : en
Pages : 141

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Book Description
Intrinsically disordered proteins lack stable 3D structures in vivo, are functionally important, and are very common in nature. In the past three decades, many studies focused on prediction of intrinsic disorder from protein sequence, estimation of its abundance, and analyses of its functional roles. However, these studies were limited in their scope; for example, they focused only on one of many functional and structural aspects. We performed first-of-its-kind comprehensive and detailed analysis of abundance, functional roles, and cellular localizations of intrinsic disorder in complete proteomes. We show that intrinsic disorder is abundant across all kingdoms of life including viruses, is involved in crucial cellular processes, such as translation, transcription, metabolism, regulation, signaling, and so on, and is preferentially located in the ribosome and nucleus. We also mapped intrinsic disorder into eukaryotic, bacterial and archaean cells. These observations motivated us to further analyze two protein families ? ribosomal proteins and proteins involved in the programmed cell death. We performed analysis across multiple species, which shows that intrinsic disorder is enriched and performs a variety of important cellular functions in ribosomal and cell death proteins. These two studies reveal that intrinsic disorder is involved in the interactions between proteins, RNAs, and DNAs. The prediction and characterization of these interactions for ordered proteins (i.e., proteins with stable 3D structures in vivo) recently attracted significant attention. However, there are no methods that target these functions/interactions mediated by the intrinsic disorder. Development of such methods is now possible by using the curated functional annotations of intrinsic disorder from the DisProt database. Utilizing these data we developed the first computational prediction method, DisoRDPbind, that predicts protein-protein, -RNA and -DNA interactions mediated by the intrinsic disorder. Our method utilizes logistic regression algorithm and a custom-designed and empirically selected set of descriptors of the input protein sequence. Empirical assessment using two benchmark datasets and large-scale predictions on four eukaryotic proteomes suggests that DisoRDPbind provides good predictive quality, differs from the methods focused on the predictions for the ordered proteins, and its computational efficiency allows for annotation of these interactions in whole proteomes.

Large-scale Characterization of Intrinsic Disorder and High-throughput Prediction Of RNA, DNA and Protein Binding Mediated by Intrinsic Disorder

Large-scale Characterization of Intrinsic Disorder and High-throughput Prediction Of RNA, DNA and Protein Binding Mediated by Intrinsic Disorder PDF Author: Zhenling Peng
Publisher:
ISBN:
Category : Bioinformatics
Languages : en
Pages : 141

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Book Description
Intrinsically disordered proteins lack stable 3D structures in vivo, are functionally important, and are very common in nature. In the past three decades, many studies focused on prediction of intrinsic disorder from protein sequence, estimation of its abundance, and analyses of its functional roles. However, these studies were limited in their scope; for example, they focused only on one of many functional and structural aspects. We performed first-of-its-kind comprehensive and detailed analysis of abundance, functional roles, and cellular localizations of intrinsic disorder in complete proteomes. We show that intrinsic disorder is abundant across all kingdoms of life including viruses, is involved in crucial cellular processes, such as translation, transcription, metabolism, regulation, signaling, and so on, and is preferentially located in the ribosome and nucleus. We also mapped intrinsic disorder into eukaryotic, bacterial and archaean cells. These observations motivated us to further analyze two protein families ? ribosomal proteins and proteins involved in the programmed cell death. We performed analysis across multiple species, which shows that intrinsic disorder is enriched and performs a variety of important cellular functions in ribosomal and cell death proteins. These two studies reveal that intrinsic disorder is involved in the interactions between proteins, RNAs, and DNAs. The prediction and characterization of these interactions for ordered proteins (i.e., proteins with stable 3D structures in vivo) recently attracted significant attention. However, there are no methods that target these functions/interactions mediated by the intrinsic disorder. Development of such methods is now possible by using the curated functional annotations of intrinsic disorder from the DisProt database. Utilizing these data we developed the first computational prediction method, DisoRDPbind, that predicts protein-protein, -RNA and -DNA interactions mediated by the intrinsic disorder. Our method utilizes logistic regression algorithm and a custom-designed and empirically selected set of descriptors of the input protein sequence. Empirical assessment using two benchmark datasets and large-scale predictions on four eukaryotic proteomes suggests that DisoRDPbind provides good predictive quality, differs from the methods focused on the predictions for the ordered proteins, and its computational efficiency allows for annotation of these interactions in whole proteomes.

Systems Medicine

Systems Medicine PDF Author:
Publisher: Academic Press
ISBN: 0128160780
Category : Science
Languages : en
Pages : 1571

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Book Description
Technological advances in generated molecular and cell biological data are transforming biomedical research. Sequencing, multi-omics and imaging technologies are likely to have deep impact on the future of medical practice. In parallel to technological developments, methodologies to gather, integrate, visualize and analyze heterogeneous and large-scale data sets are needed to develop new approaches for diagnosis, prognosis and therapy. Systems Medicine: Integrative, Qualitative and Computational Approaches is an innovative, interdisciplinary and integrative approach that extends the concept of systems biology and the unprecedented insights that computational methods and mathematical modeling offer of the interactions and network behavior of complex biological systems, to novel clinically relevant applications for the design of more successful prognostic, diagnostic and therapeutic approaches. This 3 volume work features 132 entries from renowned experts in the fields and covers the tools, methods, algorithms and data analysis workflows used for integrating and analyzing multi-dimensional data routinely generated in clinical settings with the aim of providing medical practitioners with robust clinical decision support systems. Importantly the work delves into the applications of systems medicine in areas such as tumor systems biology, metabolic and cardiovascular diseases as well as immunology and infectious diseases amongst others. This is a fundamental resource for biomedical students and researchers as well as medical practitioners who need to need to adopt advances in computational tools and methods into the clinical practice. Encyclopedic coverage: ‘one-stop’ resource for access to information written by world-leading scholars in the field of Systems Biology and Systems Medicine, with easy cross-referencing of related articles to promote understanding and further research Authoritative: the whole work is authored and edited by recognized experts in the field, with a range of different expertise, ensuring a high quality standard Digitally innovative: Hyperlinked references and further readings, cross-references and diagrams/images will allow readers to easily navigate a wealth of information

In Silico Drug Design

In Silico Drug Design PDF Author: Kunal Roy
Publisher: Academic Press
ISBN: 0128163771
Category : Medical
Languages : en
Pages : 888

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Book Description
In Silico Drug Design: Repurposing Techniques and Methodologies explores the application of computational tools that can be utilized for this approach. The book covers theoretical background and methodologies of chem-bioinformatic techniques and network modeling and discusses the various applied strategies to systematically retrieve, integrate and analyze datasets from diverse sources. Other topics include in silico drug design methods, computational workflows for drug repurposing, and network-based in silico screening for drug efficacy. With contributions from experts in the field and the inclusion of practical case studies, this book gives scientists, researchers and R&D professionals in the pharmaceutical industry valuable insights into drug design. Discusses the theoretical background and methodologies of useful techniques of cheminformatics and bioinformatics that can be applied for drug repurposing Offers case studies relating to the in silico modeling of FDA-approved drugs for the discovery of antifungal, anticancer, antiplatelet agents, and for drug therapies against diseases Covers tools and databases that can be utilized to facilitate in silico methods for drug repurposing

Genome-wide Studies of DNA and RNA with Modifications Through High-throughput Sequencing Analysis

Genome-wide Studies of DNA and RNA with Modifications Through High-throughput Sequencing Analysis PDF Author: Blythe S. Moreland
Publisher:
ISBN:
Category : Biophysics
Languages : en
Pages :

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Book Description
DNA/RNA-protein interactions are crucial to the maintenance, processing, and regulation of the genetic information contained within a cell. Sets of particular DNA/RNA-protein interactions can confer specificity to a protein's binding behavior, which makes the consideration of DNA and RNA with modifications interesting in how they alter the landscape of interactions. High-throughput sequencing (HTS) techniques of DNA and RNA can offer unmatched genome-wide characterizations of where and how proteins interact with DNA and RNA by generating libraries of millions of reads that can capture the whole distribution of these interaction events. In this dissertation we used HTS analysis techniques to probe the location and state of two nucleic acid modifications on a genome-wide scale: The methylation of Cytosines in the CpG dinucleotide (mCpG) in the human genome, and the nucleotide addition by 3'-5' polymerases to the 5'-ends of RNAs. In the case of DNA methylation, the sequencing data represents DNA fragments enriched in mCpGs by way of interaction with the methyl-CpG-binding domain (MBD) protein MBD2. In the case of 5'-end nucleotide addition, the sequencing data is a snapshot of non-coding RNAs whose 5'-ends may have been extended by a Thg1-like protein (TLP). In both sets of studies, the information about the modification in turn conveys information on the relevant DNA-protein and RNA-protein interactions, and what sequences or structures are preferred by the proteins reading or depositing the modifications. In Chapter 2, a deep sample of methylated genomic DNA allows us to characterize the sequence, spacing, and mCpG density biases introduced through MBD2 interaction during a protein pulldown experiment. In Chapter 3, we use the characterizations of those interactions -- the 3 bp minimum separation between mCpGs, the nonlinear relationship between mCpG number and pulldown efficiency -- to build a model to predict expected pulldown from a SssI Control sample, which is then used to increase the accuracy of methylation quantification from MBD pulldown data. We find that the use of our pulldown alignment model of an SssI Control data set is suitable for substitution for observed SssI Control data with use of the empirical Bayes' model BayMeth. In Chapter 4, we pivot to developing a HTS screen for unknown substrates of TLPs, BtTLP and DdiTLP4, by detecting changes in 5'-end composition under different TLP conditions. Importantly, we detect BtTLP's activity on tRNA-His, of U-1 addition, which sufficiently allows for the tRNA's essential recognition by Histidyl-tRNA synthetase (HisRS). HTS techniques and analysis will continue to improve our ability to differentiate the distributions of DNA/RNA-protein interactions between "background" and "modified" states of nucleic acids.

Dancing Protein Clouds: Intrinsically Disordered Proteins in the Norm and Pathology

Dancing Protein Clouds: Intrinsically Disordered Proteins in the Norm and Pathology PDF Author: Vladimir Uversky
Publisher: Academic Press
ISBN: 012816851X
Category :
Languages : en
Pages : 426

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Book Description
"Dancing protein clouds: Intrinsically disordered proteins in the norm and pathology" represents a set of selected studies on a variety of research topics related to intrinsically disordered proteins. Topics in this update include structural and functional characterization of several important intrinsically disordered proteins, such as 14-3-3 proteins and their partners, as well as proteins from muscle sarcomere; representation of intrinsic disorder-related concept of protein structure-function continuum; discussion of the role of intrinsic disorder in phenotypic switching; consideration of the role of intrinsically disordered proteins in the pathogenesis of neurodegenerative diseases and cancer; discussion of the roles of intrinsic disorder in functional amyloids; demonstration of the usefulness of the analysis of translational diffusion of unfolded and intrinsically disordered proteins; consideration of various computational tools for evaluation of functions of intrinsically disordered regions; and discussion of the role of shear stress in the amyloid formation of intrinsically disordered regions in the brain. Provides some recent studies on the intrinsically disordered proteins and their functions, as well as on the involvement of intrinsically disordered proteins in pthogenesis of various diseases Contains numerous illustrative materials (color figures, diagrams, and tables) to help the readers to delve in the information provided Includes contributions from recognized experts in the field

Prediction of Protein Secondary Structure

Prediction of Protein Secondary Structure PDF Author: Yaoqi Zhou
Publisher: Humana
ISBN: 9781493964048
Category : Science
Languages : en
Pages : 0

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Book Description
This thorough volume explores predicting one-dimensional functional properties, functional sites in particular, from protein sequences, an area which is getting more and more attention. Beginning with secondary structure prediction based on sequence only, the book continues by exploring secondary structure prediction based on evolution information, prediction of solvent accessible surface areas and backbone torsion angles, model building, global structural properties, functional properties, as well as visualizing interior and protruding regions in proteins. Written for the highly successful Methods in Molecular Biology series, the chapters include the kind of detail and implementation advice to ensure success in the laboratory. Practical and authoritative, Prediction of Protein Secondary Structure serves as a vital guide to numerous state-of-the-art techniques that are useful for computational and experimental biologists.

Fuzziness

Fuzziness PDF Author: Monika Fuxreiter
Publisher: Springer Science & Business Media
ISBN: 1461406595
Category : Medical
Languages : en
Pages : 210

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Book Description
Detailed characterization of fuzzy interactions will be of central importance for understanding the diverse biological functions of intrinsically disordered proteins in complex eukaryotic signaling networks. In this volume, Peter Tompa and Monika Fuxreiter have assembled a series of papers that address the issue of fuzziness in molecular interactions. These papers provide a broad overview of the phenomenon of fuzziness and provide compelling examples of the central role played by fuzzy interactions in regulation of cellular signaling processes and in viral infectivity. These contributions summarize the current state of knowledge in this new field and will undoubtedly stimulate future research that will further advance our understanding of fuzziness and its role in biomolecular interactions.

Molecular Epidemiology

Molecular Epidemiology PDF Author: Paul A. Schulte
Publisher: Academic Press
ISBN: 0323138578
Category : Medical
Languages : en
Pages : 609

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Book Description
This book will serve as a primer for both laboratory and field scientists who are shaping the emerging field of molecular epidemiology. Molecular epidemiology utilizes the same paradigm as traditional epidemiology but uses biological markers to identify exposure, disease or susceptibility. Schulte and Perera present the epidemiologic methods pertinent to biological markers. The book is also designed to enumerate the considerations necessary for valid field research and provide a resource on the salient and subtle features of biological indicators.

Protein-Nucleic Acid Interactions

Protein-Nucleic Acid Interactions PDF Author: Phoebe A. Rice
Publisher: Royal Society of Chemistry
ISBN: 0854042725
Category : Science
Languages : en
Pages : 417

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Book Description
This book provides both in-depth background and up-to-date information in this area. The chapters are organized by general themes and principles, written by experts who illustrate topics with current findings. Topics covered include: - the role of ions and hydration in protein-nucleic acid interactions - transcription factors and combinatorial specificity - indirect readout of DNA sequence - single-stranded nucleic acid binding proteins - nucleic acid junctions and proteins, - RNA protein recognition - recognition of DNA damage. It will be a key reference for both advanced students and established scientists wishing to broaden their horizons.

The Specificity of Serological Reactions

The Specificity of Serological Reactions PDF Author: Karl Landsteiner
Publisher: Courier Corporation
ISBN: 0486151441
Category : Science
Languages : en
Pages : 372

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Book Description
Nobel prizewinner's account of experiments he and colleagues carried out on antigens and serological reactions with simple compounds. Exceptionally broad coverage of basic immunology. Extensive bibliography.