Disruption of Protein-protein Interfaces and Computational Mechanistic Studies - read free eBook in online reader or directly download on the web page. Select files or add your book in reader. Download and read online ebook Disruption of Protein-protein Interfaces and Computational Mechanistic Studies write by Phillip Pierre Painter. This book was released on 2015. Disruption of Protein-protein Interfaces and Computational Mechanistic Studies available in PDF, EPUB and Kindle. Research is nothing if not collaborative; computational chemists have a wide variety of tools available at their disposal and can greatly facilitate the progress of research beyond what is possible using only traditional synthetic techniques. On the whole, computational chemistry has steadily gained acceptance in the scientific community. Advantages include no purifications of intermediates, virtually no exposure to toxic chemicals in the laboratory, and (relatively) quick turnarounds. When modeling specific reactions, the difficulty arises in interpreting the Potential Energy Surface (PES) and building a predictive model of reactivity rather than exhaustively examining every possibility. The use of computers as a tool to aid the modern chemist is examined within these chapters and explored in the context of small molecule inhibitor design and Density Functional Theory (DFT) mechanistic studies. Section 1 - Design and synthesis of potential therapeutics The rationale design of new therapeutics is a key application of computational chemistry. The chapters within this section serve as an introduction to the potential applications and utility of these methods. Chapter 1: This chapter introduces the need for new antibiotics and the basics of the computational methods used in the following chapters. Chapter 2: The design and synthesis of potential bacterial cell division modulators is explored. The need for new antibiotics is readily documented in the literature as modern antibiotics form an evolutionary pressure. Understanding the mechanisms by which bacterial cells divide, and thus propagate, could lead to novel therapeutics. SulA naturally modulates the bacterial cell division protein FtsZ, and disrupting this interaction with a small molecule allows for study without the need for inducing a genetic mutation. Two inhibitor scaffolds for disrupting this protein interface were designed using the Openeye suite of programs. Additionally, the screening of large molecular libraries from the ZINC database was accomplished against both the SulA and FtsZ protein receptors, leading to identification of commercially available compounds that could be assayed against both protein targets. Chapter 3: The generation and screening of a novel library based on Gyramide A for LogD and other molecular descriptors from commercially available benzaldehydes and sulfonamides was accomplished. Section 2 -- Pericyclic reactions Pericyclic reactions allow for complex transformations of organic skeletons in a concerted fashion, thereby preserving stereochemical information. These reactions are not only relevant to the synthetic world, but are found in nature as well. Chapter 4: The [3,3] sigmatropic shift reaction, known as the Cope rearrangement, is explored. In the addition of alkynyl sulfones and tertiary amines, ring expansion is found to be dictated largely by steric considerations, while a lone pair on carbon acts largely as a substituent instead of a nucleophile. Chapter 5: A bio-mimetic variation of the Cope rearrangement utilizing Globiferin is explored. An intriguing catalytic effect was discovered when a protonated tertiary amine was used to try to find a stepwise pathway, but a concerted process with a substantially lower barrier for rearrangement was found instead, having a potentially substantial affect on our understanding of biosynthetic pathways. Chapter 6: The viability of Nitrone-Alkene (3+2) cyclizations is explored in the formation of Fluggine A. One of the reactants can undergo a competing (3+2) cyclization intramolecularly. However, this is found to have a higher barrier. This is consistent with the observation of Fluggine A formation when the required norsecurinine substrate is present, and cyclization with itself to form virosaine B when norsecurinine is absent. Section 3 -- Synthetic Collaborations/Heterocycle reactions The projects within this section are collaborations with synthetic groups at other universities and illustrate the utility in direct collaborations between computational chemists and other researchers. Each chapter in this section covers the formation of heterocycles, which are a privileged scaffold and known to possess biologically relevant activity. As such, the formation of new heterocycles is of great scientific interest. Chapter 7: Bryostatin 1 is of biological interest due to antitumor activity, and its complex chemical structure. The formation of tetrahydropyran analogs of bryostatin 1 derived via silyl-Prins cyclization is examined computationally in this chapter. The stabilization of a tertiary cation by a [beta]-silyl substituent is key for explaining the observed selectivity. Chapter 8: The possibility of a pericyclic six-electron electrocyclization in the formation of indolines is explored but found to be significantly higher than the comparable 5-endo-trig cyclization. The competing mechanisms were found to arise from different imine reactant geometries, allowing for different orbital alignments in their respective TS geometries. The cinchona alkaloids are found to affect enantioselectivity through more than a simple counter-ion effect. Chapter 9: This chapter describes a collaborative project between three academic groups -- specialists in synthetic methods, quantum chemical computations, and kinetic studies -- to reconcile differences in data obtained while studying a heterocycloisomerization reaction for the creation of annulated aminopyrroles. Through collaboration, a complete picture of the mechanism was obtained, which would have been insufficient/inadequate had any one research group been removed.
Disruption of Protein-Protein Interfaces
Disruption of Protein-Protein Interfaces - read free eBook in online reader or directly download on the web page. Select files or add your book in reader. Download and read online ebook Disruption of Protein-Protein Interfaces write by Stefano Mangani. This book was released on 2013-06-28. Disruption of Protein-Protein Interfaces available in PDF, EPUB and Kindle. "Disruption of Protein-Protein Interfaces" reviews the latest developments and future perspectives in drug discovery at protein-protein interfaces. The authors detail experimental and computational tools to tackle the subject and highlight the contribution of the Italian research community to the field. Evidence shows that blocking or modulating protein-protein interactions might lead to the development of useful new drugs. Consequently, in recent years great effort has been dedicated to unveiling the molecular details of protein-protein interfaces by structural techniques e.g. X-ray diffraction, NMR spectroscopy. This book, written and edited by leaders in the field, provides examples from the literature of successes and failures to develop drug-like molecules effective in interacting at protein-protein interfaces.
Protein-protein Complexes
Protein-protein Complexes - read free eBook in online reader or directly download on the web page. Select files or add your book in reader. Download and read online ebook Protein-protein Complexes write by Martin Zacharias. This book was released on 2010. Protein-protein Complexes available in PDF, EPUB and Kindle. Given the immense progress achieved in elucidating protein-protein complex structures and in the field of protein interaction modeling, there is great demand for a book that gives interested researchers/students a comprehensive overview of the field. This book does just that. It focuses on what can be learned about protein-protein interactions from the analysis of protein-protein complex structures and interfaces. What are the driving forces for protein-protein association? How can we extract the mechanism of specific recognition from studying protein-protein interfaces? How can this knowledge be used to predict and design protein-protein interactions (interaction regions and complex structures)? What methods are currently employed to design protein-protein interactions, and how can we influence protein-protein interactions by mutagenesis and small-molecule drugs or peptide mimetics?The book consists of about 15 review chapters, written by experts, on the characterization of protein-protein interfaces, structure determination of protein complexes (by NMR and X-ray), theory of protein-protein binding, dynamics of protein interfaces, bioinformatics methods to predict interaction regions, and prediction of protein-protein complex structures (docking and homology modeling of complexes, etc.) and design of protein-protein interactions. It serves as a bridge between studying/analyzing protein-protein complex structures (interfaces), predicting interactions, and influencing/designing interactions.
Protein-Protein Interactions
Protein-Protein Interactions - read free eBook in online reader or directly download on the web page. Select files or add your book in reader. Download and read online ebook Protein-Protein Interactions write by Krishna Mohan Poluri. This book was released on 2021-05-19. Protein-Protein Interactions available in PDF, EPUB and Kindle. This book provides a comprehensive overview of the fundamental aspects of protein-protein interactions (PPI), including a detailed account of the energetics and thermodynamics involved in these interactions. It also discusses a number of computational and experimental approaches for the prediction of PPI interactions and reviews their principles, advantages, drawbacks, and the recent developments. Further, it offers structural and mechanistic insights into the formation of protein-protein complexes and maps different PPIs into networks to delineate various pathways that operate at the cellular level. Lastly, it describes computational protein-protein docking techniques and discusses their implications for further experimental research. Given its scope, this book is a valuable resource for students, researchers, scientists, entrepreneurs, and medical/healthcare professionals.
Mechanistic Studies of Protein-protein Interaction and Replication Initiation
Mechanistic Studies of Protein-protein Interaction and Replication Initiation - read free eBook in online reader or directly download on the web page. Select files or add your book in reader. Download and read online ebook Mechanistic Studies of Protein-protein Interaction and Replication Initiation write by Yabin Lu. This book was released on 1998. Mechanistic Studies of Protein-protein Interaction and Replication Initiation available in PDF, EPUB and Kindle.
