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Book Targeting Unique Nucleic Acid Structures with Small Molecules

Download or read book Targeting Unique Nucleic Acid Structures with Small Molecules written by Victor Kin-man Tam and published by . This book was released on 2007 with total page 217 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Book Effect of Small Molecules on Nucleic Acid Stability and Improvements to RNA Structure Prediction

Download or read book Effect of Small Molecules on Nucleic Acid Stability and Improvements to RNA Structure Prediction written by Kehinde Sowunmi and published by GRIN Verlag. This book was released on 2020-07-14 with total page 32 pages. Available in PDF, EPUB and Kindle. Book excerpt: Academic Paper from the year 2020 in the subject Biology - Genetics / Gene Technology, grade: 9.0, , course: Cell Biology and Genetics, language: English, abstract: Nucleic acids have proven to be viable targets for small molecule drugs. While many examples of such drugs are detailed in the literature, only a select few have found practical use in a clinical setting. These currently employed nucleic acid targeting therapies suffer from either debilitating off-target side effects or succumb to a resistance mechanism of the target. The need for new small molecules that target nucleic acids is evident. However, designing a novel drug to bind to DNA or RNA requires a detailed understanding of exactly what binding environments each nucleic acid presents. In an effort to broaden this knowledge, the work presented in this thesis details the binding location and affinity of known and novel nucleic acid binding small molecules with targets ranging from simple RNA secondary structure all the way to the complex structure of ribosomal RNA. Specifically, it is shown that the anthracycline classes of antineoplastics prefer to bind at or near mismatch base pairs in both physiologically relevant iron responsive element RNA hairpin constructs as well as DNA hairpin constructs presenting mismatched base pairs. Also characterized in this thesis is a novel class of topoisomerase II / histone deacetylase inhibitor conjugates that display a unique affinity for DNA over RNA. Finally, the novel class of macrolide-peptide conjugates, known as peptolides, is shown to retain potent translation inhibition of the prokaryotic ribosome and identification of a novel binding site for the anthracycline class of drugs and the characterization of the two novel drug designs presented in this thesis will undoubtedly aid in the effort to design and discover new molecules that aim for nucleic acid targets.

Book Interaction of Small Molecules with Nucleic Acid Targets

Download or read book Interaction of Small Molecules with Nucleic Acid Targets written by Joshua Craig Canzoneri and published by . This book was released on 2012 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: Nucleic acids have proven to be viable targets for small molecule drugs. While many examples of such drugs are detailed in the literature, only a select few have found practical use in a clinical setting. These currently employed nucleic acid targeting therapies suffer from either debilitating off-target side effects or succumb to a resistance mechanism of the target. The need for new small molecules that target nucleic acids is evident. However, designing a novel drug to bind to DNA or RNA requires a detailed understanding of exactly what binding environments each nucleic acid presents. In an effort to broaden this knowledge, the work presented in this thesis details the binding location and affinity of known and novel nucleic acid binding small molecules with targets ranging from simple RNA secondary structure all the way to the complex structure of ribosomal RNA. Specifically, it is shown that the anthracycline class of antineoplastics prefer to bind at or near mismatch base pairs in both physiologically relevant iron responsive element RNA hairpin constructs as well as DNA hairpin constructs presenting mismatched base pairs. Also characterized in this thesis is a novel class of topoisomerase II / histone deacetylase inhibitor conjugates that display a unique affinity for DNA over RNA. Finally, the novel class of macrolide-peptide conjugates, known as peptolides, are shown to retain potent translation inhibition of the prokaryotic ribosome. The binding pocket of the peptolides, including a crevice previously unreachable by macrolides that extends away from the peptidyl transferase center toward the subunit interface, is confirmed in detail via chemical footprinting of the 70S ribosome. Overall, the identification of a novel binding site for the anthracycline class of drugs and the characterization of the two novel drug designs presented in this thesis will undoubtedly aid in the effort to design and discover new molecules that aim for nucleic acid targets. For example, the anthracycline derivative topoisomerase II / histone deacetylase inhibitor conjugates, with their differential mode of nucleic acid binding, may prove to have a unique side effect profile in a therapeutic application. The peptolide compounds also have the potential to be applied as novel antibiotics as they bind to an area of the prokaryotic ribosome unrelated to known macrolide resistance mutations. Furthermore, as a result of the observation of this thesis work that some peptolides also posses eukaryotic translation inhibition capabilities, they could prove to be useful in preventing the growth of rapidly proliferating eukaryotic cells such as plasmodium, leishmania, or tumor cells. Additionally, different head groups could be utilized in creating new peptolides; for example, an oxazolidinone antibiotic could be employed to sample a different binding area of the ribosome.

Book Selective Targeting of Nucleic Acids by Small Molecules

Download or read book Selective Targeting of Nucleic Acids by Small Molecules written by Caterina Musetti and published by . This book was released on 2011 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Book RNA as a Drug Target

    Book Details:
  • Author : John Schneekloth
  • Publisher : John Wiley & Sons
  • Release : 2024-10-07
  • ISBN : 3527351000
  • Pages : 418 pages

Download or read book RNA as a Drug Target written by John Schneekloth and published by John Wiley & Sons. This book was released on 2024-10-07 with total page 418 pages. Available in PDF, EPUB and Kindle. Book excerpt: Discover a new paradigm in drug discovery that greatly expands the space of addressable drug targets and potential novel drugs Existing paradigms for drug discovery have focused largely on enzymes and other proteins as drug targets. In recent years, however, different varieties of ribonucleic acids have emerged as a viable focus for target-based drug discovery, with the potential to revolutionize the strategy and approach for this essential step in the drug development process. RNA as a Drug Target: The Next Frontier for Medicinal Chemistry offers a practice-oriented introduction to developing drug-like small molecules that selectively modulate both coding and non-coding RNAs. Beginning with a description and characterization of existing druggable RNAs, the book discusses how to approach different RNA targets for drug discovery. The result is a crucial resource for targeting RNAs and creating the next generation of life-saving pharmaceuticals. RNA as a Drug Target readers will also find: A complete “toolbox” for working with RNA, from structure determination to screening and lead generation techniques A wide range of addressable targets and mechanisms, including splicing modulation, riboswitches, targeted degradation, and more Authoritative discussion of the potential of RNA-targeted small molecule therapeutics for drugging the epitranscriptome RNA as a Drug Target provides an expert introduction to a new frontier in pharmaceutical research for medicinal chemists, biochemists, molecular biologists, and members of the pharmaceutical industry.

Book Long Non Coding RNA Biology

Download or read book Long Non Coding RNA Biology written by M.R.S. Rao and published by Springer. This book was released on 2017-08-16 with total page 336 pages. Available in PDF, EPUB and Kindle. Book excerpt: This contributed volume offers a comprehensive and detailed overview of the various aspects of long non-coding RNAs and discusses their emerging significance. Written by leading experts in the field, it motivates young researchers around the globe, and offers graduate and postgraduate students fascinating insights into genes and their regulation in eukaryotes and higher organisms.

Book Small Molecule DNA and RNA Binders

Download or read book Small Molecule DNA and RNA Binders written by Martine Demeunynck and published by John Wiley & Sons. This book was released on 2006-03-06 with total page 754 pages. Available in PDF, EPUB and Kindle. Book excerpt: The development of molecules that selectively bind to nucleic acids has provided many details about DNA and RNA recognition. The range of such substances, such as metal complexes, peptides, oligonucleotides and a wide array of synthetic organic compounds, is as manifold as the functions of nucleic acids. Nucleic acid recognition sequences are often found in the major or minor groove of a double strand, while other typical interactions include intercalation between base pairs or the formation of triple or quadruple helices. One example of a binding mode that has recently been proposed is end stacking on such complex structures as the telomere tetraplex. In this comprehensive book, internationally recognized experts describe in detail the important aspects of nucleic acid binding, and in so doing present impressive approaches to drug design. Since typical substances may be created naturally or synthetically, emphasis is placed on natural products, chemical synthesis, the use of combinatorial libraries, and structural characterization. The whole is rounded off by contributions on molecular modeling, as well as investigations into the way in which any given drug interacts with its nucleic acid recognition site.

Book DNA targeting Molecules as Therapeutic Agents

Download or read book DNA targeting Molecules as Therapeutic Agents written by Michael J. Waring and published by Royal Society of Chemistry. This book was released on 2018-03-12 with total page 432 pages. Available in PDF, EPUB and Kindle. Book excerpt: There have been remarkable advances towards discovering agents that exhibit selectivity and sequence-specificity for DNA, as well as understanding the interactions that underlie its propensity to bind molecules. This progress has important applications in many areas of biotechnology and medicine, notably in cancer treatment as well as in future gene targeting therapies. The editor and contributing authors are leaders in their fields and provide useful perspectives from diverse and interdisciplinary backgrounds on the current status of this broad area. The role played by chemistry is a unifying theme. Early chapters cover methodologies to evaluate DNA-interactive agents and then the book provides examples of DNA-interactive molecules and technologies in development as therapeutic agents. DNA-binding metal complexes, peptide and polyamide–DNA interactions, and gene targeting tools are some of the most compelling topics treated in depth. This book will be a valuable resource for postgraduate students and researchers in chemical biology, biochemistry, structural biology and medicinal fields. It will also be of interest to supramolecular chemists and biophysicists.

Book Synthesis of Small Molecules Targeting RNA

Download or read book Synthesis of Small Molecules Targeting RNA written by Qi Liu and published by . This book was released on 2004 with total page 370 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Book Principles of Nucleic Acid Structure

Download or read book Principles of Nucleic Acid Structure written by Stephen Neidle and published by Academic Press. This book was released on 2021-10-15 with total page 456 pages. Available in PDF, EPUB and Kindle. Book excerpt: Principles of Nucleic Acid Structure, Second Edition, provides the most complete and concise summary of underlying principles and approaches to studying nucleic acid structure, including discussions of X-ray crystallography, NMR, molecular modelling and databases. The book's focus is on a survey of structures that are especially important for biomedical research and pharmacological applications. This updated edition includes the latest advances relevant to recognition of DNA and RNA by small molecules and proteins, including sections on RNA folding, ribosome structure and antibiotic interactions, DNA quadruplexes, DNA and RNA protein complexes and short interfering RNA (siRNA). This reference is a must-have for those seeking an authoritative, comprehensive and up-to-date source on all aspects of nucleic acid structure, from basic first principles to details of recent research results. Completely updated, with an expanded section on protein-nucleic acid interactions that reflects major increases in our knowledge Defines technical terms for novices Includes a complete list of resources, including relevant online databases and software, as well as useful websites

Book Analysis and Effect of Small molecules Targeting Pre microRNA Structures and Synthetic Efforts Toward a Novel Scaffold for RNA Targeting

Download or read book Analysis and Effect of Small molecules Targeting Pre microRNA Structures and Synthetic Efforts Toward a Novel Scaffold for RNA Targeting written by Oliver Leonard Rayborn Swart and published by . This book was released on 2019 with total page 176 pages. Available in PDF, EPUB and Kindle. Book excerpt: "The growing understanding of functional non-coding RNA has seen a sharp rise in the importance of RNA both as a player in functional biology and for its role in the manifestation of many types of disease. This has stimulated the need for design and discovery of small molecules that can specifically interact with RNAs, for use as chemical probes and therapeutics. However, there is difficulty in the production of these molecules as the "rules" which govern the specific RNA interactions are not fully understood. This thesis discusses the application of a resin-bound dynamic combinatorial library (RBDCL) in the discovery of molecules which possess affinity and specificity toward unique RNA structures, as well as the modification and analysis of such molecules as RNA ligands in vitro and in celluo. Moreover, a novel RNA-focused small molecule library is proposed, centered about the use of a 2,5-diketopiperazine (DKP) chemical scaffold. Synthetic routes to this structure and their utility in exploring chemical diversity are discussed. Toward the utility of an RBDCL in evolving RNA binding molecules, an approach was carried out using the premature forms of microRNAs 21 and 96 as targets for small molecule interaction. In their mature states, both of these RNAs function as oncogenes in many forms of cancer. Derived molecules demonstrate ability to bind preferentially to a specific premature structure with strong affinities. Enzymatic studies performed in vitro elucidate the utility of the molecules binding modes in preventing the generation of the mature RNAs at low micromolar concentrations. In cancer cell cultures, treatment with these molecules corresponds to increases in apoptotic events, suggesting reinstated tumor suppressor function through microRNA inhibition. Apoptosis observed with treatment also displays an additive effect when treated with cell death related cytokines or chemotherapeutics. Heterocyclic substructures, particularly those with rod-like orienting ability, have displayed a high degree of utility in the generation of RNA-preferenced small molecules. The 2,5-diketopiperazaine is a synthetically simple heterocycle with a notable pedigree in biologically active molecules. Surprisingly, this molecular scaffold has as yet never been targeted to RNA structure interaction. Synthetic pathways to differentially substituted DKPs are explored both in solution and on solid-phase for application to a dynamic library. Analysis of the RNA interacting capability of the DKP scaffold was performed through the use of a previously known RNA-binding molecule. A mono-quinoline analogue containing a DKP structure was able to bind the HIV-1 frameshift stimulatory sequence of RNA with affinity comparable to the non-DKP molecules despite the loss of a quinoline heterocycle. This is the first instance demonstrating a 2,5-diketopiperazine containing molecule participating in RNA binding"--Pages viii-ix.

Book De novo Molecular Design

    Book Details:
  • Author : Gisbert Schneider
  • Publisher : John Wiley & Sons
  • Release : 2013-10-10
  • ISBN : 3527677038
  • Pages : 540 pages

Download or read book De novo Molecular Design written by Gisbert Schneider and published by John Wiley & Sons. This book was released on 2013-10-10 with total page 540 pages. Available in PDF, EPUB and Kindle. Book excerpt: Systematically examining current methods and strategies, this ready reference covers a wide range of molecular structures, from organic-chemical drugs to peptides, Proteins and nucleic acids, in line with emerging new drug classes derived from biomacromolecules. A leader in the field and one of the pioneers of this young discipline has assembled here the most prominent experts from across the world to provide first-hand knowledge. While most of their methods and examples come from the area of pharmaceutical discovery and development, the approaches are equally applicable for chemical probes and diagnostics, pesticides, and any other molecule designed to interact with a biological system. Numerous images and screenshots illustrate the many examples and method descriptions. With its broad and balanced coverage, this will be the firststop resource not only for medicinal chemists, biochemists and biotechnologists, but equally for bioinformaticians and molecular designers for many years to come. From the content: * Reaction-driven de novo design * Adaptive methods in molecular design * Design of ligands against multitarget profiles * Free energy methods in ligand design * Fragment-based de novo design * Automated design of focused and target family-oriented compound libraries * Molecular de novo design by nature-inspired computing * 3D QSAR approaches to de novo drug design * Bioisosteres in de novo design * De novo design of peptides, proteins and nucleic acid structures, including RNA aptamers and many more.

Book Manfred Egender

    Book Details:
  • Author : Manfred Egender
  • Publisher :
  • Release : 1992
  • ISBN : 9783906143026
  • Pages : 14 pages

Download or read book Manfred Egender written by Manfred Egender and published by . This book was released on 1992 with total page 14 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Book Principles of Nucleic Acid Structure

Download or read book Principles of Nucleic Acid Structure written by Wolfram Saenger and published by Springer Science & Business Media. This book was released on 2013-12-01 with total page 574 pages. Available in PDF, EPUB and Kindle. Book excerpt: New textbooks at all levels of chemistry appear with great regularity. Some fields like basic biochemistry, organic reaction mechanisms, and chemical ther modynamics are well represented by many excellent texts, and new or revised editions are published sufficiently often to keep up with progress in research. However, some areas of chemistry, especially many of those taught at the grad uate level, suffer from a real lack of up-to-date textbooks. The most serious needs occur in fields that are rapidly changing. Textbooks in these subjects usually have to be written by scientists actually involved in the research which is advancing the field. It is not often easy to persuade such individuals to set time aside to help spread the knowledge they have accumulated. Our goal, in this series, is to pinpoint areas of chemistry where recent progress has outpaced what is covered in any available textbooks, and then seek out and persuade experts in these fields to produce relatively concise but instructive introductions to their fields. These should serve the needs of one semester or one quarter graduate courses in chemistry and biochemistry. In some cases the availability of texts in active research areas should help stimulate the creation of new courses. CHARLES R. CANTOR New York Preface This monograph is based on a review on polynucleotide structures written for a book series in 1976.

Book Development of Nucleic Acid Targeting Molecules

Download or read book Development of Nucleic Acid Targeting Molecules written by Fai Alkathiri and published by . This book was released on 2019 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: Molecular docking is a widely used and effective structure-based computational strategy for predicting dynamics between ligands and receptors. Until now the docking software were developed for the protein-ligand interactions and very few docking tools were developed exclusively for the docking of small molecules on the nucleic acid structures like the DNA and RNA. The progress in algorithms and the need for deeper understanding of ligand-nucleic acid interactions more focused, and specialized tools are being developed to explore this hindered area of drug discovery. This chapter is focused on and discus in details about various tools available for docking with nucleic acids and how the rejuvenation of machine learning methods is making its impact on the development of these docking programs.

Book Molecular Targeting of Nucleic Acid Secondary Structures

Download or read book Molecular Targeting of Nucleic Acid Secondary Structures written by Mikkel Stockendahl Christensen and published by . This book was released on 2007 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Book Small Molecule Transcription Factor Inhibitors in Oncology

Download or read book Small Molecule Transcription Factor Inhibitors in Oncology written by Khondaker Miraz Rahman and published by Royal Society of Chemistry. This book was released on 2018-09-06 with total page 214 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book highlights recent progress in the development of small-molecule inhibitors of oncogenic transcription factors and is relevant for postgraduates, researchers and practitioners.