Structural Characterization of Complex Biological Systems Via Ultraviolet Photodissociation Mass Spectrometry

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ISBN 13 :
Total Pages : 552 pages
Book Rating : 4.:/5 (125 download)

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Book Synopsis Structural Characterization of Complex Biological Systems Via Ultraviolet Photodissociation Mass Spectrometry by : Christopher Martin Crittenden

Download or read book Structural Characterization of Complex Biological Systems Via Ultraviolet Photodissociation Mass Spectrometry written by Christopher Martin Crittenden and published by . This book was released on 2019 with total page 552 pages. Available in PDF, EPUB and Kindle. Book excerpt: The work detailed in this dissertation describes the advantages that 193 nm ultraviolet photodissociation (UVPD) affords for characterization of structurally complex biological molecules as compared to traditional ion activation techniques, such as collisional or electron-based dissociation, for mass spectrometry. UVPD, either alone or in tandem with collisional activation such as collision induced dissociation (CID), consistently provides more extensive structural information about biomolecules. One such system where the utility of both UVPD and CID was employed was in the structural characterization of lipid A species. Lipid A, the innermost structural component of lipopolysaccharides (LPS) which decorate the surface of Gram-negative bacteria, may undergo covalent modifications in order to provide resistance to antibiotics. By utilizing a combinatorial approach, CID is able to characterize the covalent modifications that are present while UVPD is able to elucidate which side of the molecule (reducing or nonreducing end) undergoes the modification through selective fragmentation of the diglucosamine backbone. This approach confirmed the presence of aminoarabinose modification present on the LPS of A. baumannii after exposure to the antibiotic polymyxin B. Another instance of utilizing the power of both photodissociation and collisional activation was in the characterization of oligosaccharide molecules from LPS of E. coli. These biomolecules are typically heavily phosphorylated near the reducing end of the saccharide backbone, and as such, collisional activation produces fragment ions originated from cleavages localized near the phosphate sites. UVPD of the oligosaccharides produces a plethora of diagnostic fragment ions throughout the molecule, but this often leads to spectral congestion and ambiguous fragment assignment. UVPD generates charge-reduced precursor ions that can be subjected to subsequent collisional activation in a MS3 event, allowing complete characterization significantly fewer confounding product ions as compared to UVPD alone. Another hallmark of UVPD is its fast, high energy deposition that causes cleavage of covalent bonds while allowing survival of non-covalent interactions. This characteristic allows electrostatic interactions to be mapped in non-covalent complexes, unlike the collisional activation which preferentially cleaves weak non-covalent interactions owing to the stepwise nature of collisional activation. In this work, it is demonstrated that UVPD of the electrostatic complex between a cationic antimicrobial peptides (CAMP) and Kdo2-lipid A illuminates, through the production of diagnostic holo peptide fragment ions retaining the intact mass of the lipid A species, which amino acids in the peptide sequence are responsible for mediating the interaction between the two molecules in the gas phase. In contrast, collisional activation of the electrostatic complex between the two species simply results in the disruption of the network of non-covalent interactions, only yielding apo peptide product ions. In the same vein, this notion of retention of electrostatic interactions post-photodissociation was employed to interrogate where metal ions were sequestered in proteins. UVPD has previously been touted as a means to determine the binding location of ligands (such as drug molecules) to proteins after transporting the protein-ligand complexes to the gas-phase by native ESI. This methodology was extended to determine the binding location of metal ions (such as calcium, copper, silver, and praseodymium, to name a few) to proteins. The binding sites of calcium (II) and a series of lanthanide (III) ions were successfully determined for staphylococcal nuclease, the binding sites of silver (I) and copper (II) were determined for azurin, and multiple binding sites for calcium (II) and select lanthanides (III) were determined for calmodulin, all agreeing with reported crystal structure data. These are but only a few examples of the utility of UVPD as an alternative to ion activation in the gas phase. The unprecedented characterization of ions by UVPD, regardless of polarity, number of charges, size of the molecule, or molecular interactions present, suggests that there are many other potential applications of UVPD in the future

Development of Top-down Mass Spectrometry Methods for Structural Characterization of Protein Macromolecules Utilizing 193nm Ultraviolet Photodissociation

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ISBN 13 :
Total Pages : 322 pages
Book Rating : 4.:/5 (15 download)

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Book Synopsis Development of Top-down Mass Spectrometry Methods for Structural Characterization of Protein Macromolecules Utilizing 193nm Ultraviolet Photodissociation by : Michael B. Cammarata

Download or read book Development of Top-down Mass Spectrometry Methods for Structural Characterization of Protein Macromolecules Utilizing 193nm Ultraviolet Photodissociation written by Michael B. Cammarata and published by . This book was released on 2016 with total page 322 pages. Available in PDF, EPUB and Kindle. Book excerpt: The dissertation will discuss the advancement of informative structural biology techniques utilizing a top-down centric workflow with 193nm ultraviolet photodissociation (UVPD) mass spectrometry. Native electrospray ionization is used to transport proteins to the gas phase in a native-like state, then UVPD is used for structural characterization to reveal ligand binding sites within a protein-ligand complex as well as detect conformational changes based upon the suppression or enhancement of backbone cleavages. Conformational changes induced by ligand exchange or removal and single amino acid mutations as well as combinations of the two (ligands and mutations) are investigated. The rich fragmentation patterns of UVPD are also used for structural characterization of crosslinked proteins. Typically these crosslinking experiments are performed by bottom-up mass spectrometry with has significant shortcomings. The main drawback is the need for proteolysis which cuts proteins into small peptides, thus increasing the complexity of the samples and its subsequent analysis. Additionally this proteolysis step loses the post-translation modification information or amino acid mutations that may be driving a specific protein-protein interaction. Top-down methods avoid protein digestion and thus are used to directly evaluate the protein interactions or protein complexes. These two methodologies will bring the mass spectrometry and structural biology community a step closer to the realization of high-throughput structural biology for proteins and their interactions with other proteins and small molecules.

Leveraging Native Mass Spectrometry and 193 Nm Ultraviolet Photodissociation as Structural Biology Tools

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ISBN 13 :
Total Pages : 726 pages
Book Rating : 4.:/5 (124 download)

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Book Synopsis Leveraging Native Mass Spectrometry and 193 Nm Ultraviolet Photodissociation as Structural Biology Tools by : Megan Rachel Mehaffey

Download or read book Leveraging Native Mass Spectrometry and 193 Nm Ultraviolet Photodissociation as Structural Biology Tools written by Megan Rachel Mehaffey and published by . This book was released on 2020 with total page 726 pages. Available in PDF, EPUB and Kindle. Book excerpt: Structural biology studies aimed at the elucidation of protein-dependent disease mechanisms have traditionally relied on high-resolution techniques, including X-ray crystallography, nuclear magnetic resonance, and cryogenic electron microscopy. While such methodologies remain standard for gaining information on the core structure of proteins, specific drawbacks including time or large sample quantities associated with these approaches have spawned the development of other pipelines. Mass spectrometry (MS) is one such tool that has gained traction as a rapid and sensitive low-resolution structural biology technique. Routinely protein complexes of interest are reacted in solution with covalent chemical probes to preserve structural information prior to enzymatic digestion and mass spectrometric read-out. However, with the advent of native MS, protein complexes can now be efficiently transferred intact into the gas phase using high ionic strength solutions while retaining structures reminiscent of their solution conformations, and directly interrogated using MS/MS methods. Ultraviolet photodissociation (UVPD) is one such ion activation method that has been extensively developed to break apart protein complexes in a manner that allows conclusions about structure to be drawn based on the fragmentation behavior. The work presented here leverages native mass spectrometry in conjunction with 193 nm UVPD to probe a variety of biologically important protein-ligand and protein-protein complexes. The utility in a native UVPD-MS approach for structural examination of protein-ligand complexes is demonstrated through characterization of conformational changes associated with the catalytic cycle of a phosphotransferase enzyme as well as elucidation of structural changes resulting from mutation or inhibition of an enzyme responsible for conferring antibiotic resistance to bacteria. An oncogenic protein and several clinical variants bound to a downstream effector protein provides an example of the capabilities of native MS and UVPD to characterize the structure of a protein-protein complex. Native UVPD-MS is also used for epitope mapping of the main antigenic determinant of the influenza virus. Aimed at improving analysis of larger complexes, multistage native UVPD-MS is developed to probe the structure of a protein implicated in chemotherapeutic resistance in glioblastoma tumors. Lastly, uniting on-line capillary electrophoresis (CE) with multistage native UVPD-MS offers a high-throughput workflow for structural characterization of ribosomal protein complexes

Development of Ultraviolet Photodissociation Mass Spectrometry Strategies for the Characterization of Biomolecular Structure

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ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (134 download)

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Book Synopsis Development of Ultraviolet Photodissociation Mass Spectrometry Strategies for the Characterization of Biomolecular Structure by : Luis Antonio Macias

Download or read book Development of Ultraviolet Photodissociation Mass Spectrometry Strategies for the Characterization of Biomolecular Structure written by Luis Antonio Macias and published by . This book was released on 2022 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: Ultraviolet photodissociation (UVPD) is an alternative high-energy ion activation technique implemented to produce information rich tandem mass spectra. Dissociation of biomolecules by UVPD results in structure dependent fragmentation to reveal molecular details that are otherwise undiscernible by traditional tandem mass spectrometry techniques, providing an avenue to rapidly interrogate the structure-function relationship of biologically relevant species. Applied to glycerophospholipids, UVPD is capable of resolving locations of unsaturation and stereospecific numbering of acyl chains, subtle structural features that are traditionally challenging to resolve. In the analysis of intact proteins, UVPD produces excellent sequence coverage that can pinpoint sites of post translational modifications, while providing conformation sensitive fragmentation that also informs changes in higher-order structure that occur upon ligand binding or mutations. Studies covered in this work extend the unique capabilities of UVPD to characterize increasingly complex molecules, explore associations between UVPD resolved structure and disease, and develop an understanding of dissociation mechanisms that govern fragmentation induced by 193 nm photons. Here, the high versatility of this technique was applied to the detailed structural characterization of cardiolipins at the double bond and stereochemistry level by utilizing hybrid techniques that combine collisional activation with UVPD; similarly, UVPD was integrated to both imaging and chromatographic workflows to evaluate fatty acid structure and phosphatidylcholine structure, respectively, as a function of disease state; furthermore, fragmentation of intact proteins was evaluated to discern mechanisms that influence photon-induced dissociation and leveraged to assign paratopes and interpret complex top-down spectra of proteins with disulfide bonds

Mass Spectrometry of Biological Materials, Second Edition

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Publisher : CRC Press
ISBN 13 : 9780824701574
Total Pages : 490 pages
Book Rating : 4.7/5 (15 download)

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Book Synopsis Mass Spectrometry of Biological Materials, Second Edition by : Barbara S. Larsen

Download or read book Mass Spectrometry of Biological Materials, Second Edition written by Barbara S. Larsen and published by CRC Press. This book was released on 1998-03-02 with total page 490 pages. Available in PDF, EPUB and Kindle. Book excerpt: Second Edition provides up-to-the-minute discussions on the application of mass spectrometry to the biological sciences. Shows how and why experiments are performed and furnishes details to facilitate duplication of results.

Development of Ultraviolet Photodissociation Based Tandem Mass Spectrometry Methods for the Characterization of Protein Macromolecular Structures and Glycolipids

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ISBN 13 :
Total Pages : 616 pages
Book Rating : 4.:/5 (919 download)

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Book Synopsis Development of Ultraviolet Photodissociation Based Tandem Mass Spectrometry Methods for the Characterization of Protein Macromolecular Structures and Glycolipids by : John Patrick O'Brien

Download or read book Development of Ultraviolet Photodissociation Based Tandem Mass Spectrometry Methods for the Characterization of Protein Macromolecular Structures and Glycolipids written by John Patrick O'Brien and published by . This book was released on 2014 with total page 616 pages. Available in PDF, EPUB and Kindle. Book excerpt: Photon-based tandem mass spectrometry provides a versatile ion activation strategy for the analysis of polypeptides, proteins, and lipids. 351-nm ultraviolet photodissociation mass spectrometry (UVPD-MS) is a facile and selective tandem dissociation technique used to elucidate chromophore-modified peptides within large mixtures. A bis-aryl chromogenic chemical probe was utilized to target solvent exposed primary amine residues within native protein states. Collision-induced dissociation (CID) was employed to indiscriminatly characterize the complete proteolytic digest while chromophore containing peptides were selectively dissociated with 351-nm UVPD; thus streamlining the identification of targeted peptides with structurally informative residues. Protein amine residue reactivities were then compared with predicted solvent exposures to elucidate protein tertiary structures, their mechanistic properties, and ligand-binding interactions. High-energy 193-nm UVPD is a fast, high-energy tandem mass spectrometry method and frequently generates fragment ions typically inaccessible to CID-based methods. Native mass spectrometry was coupled to top-down 193-nm UVPD for the gas phase characterization of non-covalent protein-ligand and protein-protein complexes. This method yielded a unique array of fragment ions for a comprehensive analysis of protein structures. UVPD of non-covalent complexes generated many polypeptide backbone fragments to characterize the primary sequence of proteins. Furthermore, top-down UVPD engendered cleavages with intact electrostatic interactions; this provided insight into the binding interfaces within protein-ligand complexes and the higher order structural architectures of oligomeric complexes. High-resolution 193-nm UVPD was paired with high performance liquid chromatography (LC) for the streamlined structural analysis of amphiphilic glycolipids within complex mixtures. For all glycolipids, UVPD provided the most comprehensive structural analysis tool by affording a diverse array of fragment ions to characterize both hydrophobic and hydrophilic moieties. UVPD based LC-MS separations of gangliosides shed light on the ceramide lipid bases, glycan moieties, and their isobaric structural variants. UVPD activation of lipid A and lipooligosaccharides (LOS) compounds generated a mixture of C-C, C-O, and C-N fragment ions to illustrate the hydrophobic acyl structures, while cleavages within the glycosidic, and cross-ring cleavages allowed the determination of acylation patterns. Novel LC-MS separation strategies were developed to elucidate and structurally characterize complex mixtures of lipopolysaccharide containing compounds.

Biofunctional Molecule Discovery and Characterization Via Multifaceted Mass Spectrometry Approaches

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ISBN 13 :
Total Pages : 156 pages
Book Rating : 4.:/5 (118 download)

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Book Synopsis Biofunctional Molecule Discovery and Characterization Via Multifaceted Mass Spectrometry Approaches by : Qinjingwen Cao

Download or read book Biofunctional Molecule Discovery and Characterization Via Multifaceted Mass Spectrometry Approaches written by Qinjingwen Cao and published by . This book was released on 2019 with total page 156 pages. Available in PDF, EPUB and Kindle. Book excerpt: Biofunctional molecules, such as neurotransmitters, metabolites and neuropeptides, are involved in various biological and regulatory processes and play essential roles in vivo. Owing to their complex structures and wide range of concentrations, analyzing those molecules in complex biological matrices has been challenging, and it is highly desirable to develop selective and sensitive analytical methodologies to achieve efficient characterization. In this dissertation, both liquid chromatography-mass spectrometry (LC-MS) and matrix-assisted laser desorption/ionization (MALDI) mass spectrometry imaging (MSI) methods were developed to identify and characterize biofunctional molecules. Specifically, an LC-MS workflow was developed to determine neurotransmitters and metabolites with a reference tandem mass spectrometry library. Moreover, an enrichment-free method has been applied to discover N-linked and O-linked glycosylation on crustacean neuropeptides. Additionally, this work demonstrates complementary MALDI MSI approaches to map in situ neurotransmitter distribution on high resolution-accurate mass Orbitrap platform. The employment of sub-atmospheric pressure MALDI MSI has featured the alleviation of ion suppression effects and produced high resolution molecular imaging of neuropeptides and lipids in vivo. Overall, this work not only improves multifaceted analytical techniques for uncovering the complexity of crustacean signaling molecules but also provides potential applications in a broad set of biological systems.

Development and Application of Methods Towards the Structural Characterization of Gas-phase Biomolecular Assemblies

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ISBN 13 :
Total Pages : 978 pages
Book Rating : 4.:/5 (133 download)

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Book Synopsis Development and Application of Methods Towards the Structural Characterization of Gas-phase Biomolecular Assemblies by : Sarah Natalie Sipe

Download or read book Development and Application of Methods Towards the Structural Characterization of Gas-phase Biomolecular Assemblies written by Sarah Natalie Sipe and published by . This book was released on 2022 with total page 978 pages. Available in PDF, EPUB and Kindle. Book excerpt: The utility of ultraviolet photodissociation mass spectrometry (UVPD-MS) in native MS approaches, including ion mobility spectrometry (IMS), for protein complexes is described in this dissertation. A modular drift tube demonstrated suitability for measuring collision cross sections (CCSs) of native-like ions on an Orbitrap mass spectrometer with high resolution using acquisition times as short as one minute. This IMS method is used throughout this dissertation for measurement of native-like and disordered structures. A fundamental study for determining the charge-dependent behavior of UVPD for protein complexes was evaluated using the homomeric Cu/Zn superoxide dismutase dimer, streptavidin tetramer, transthyretin tetramer, and C reactive protein pentamer as well as the heteromeric hemoglobin tetramer. A wide range of charge states were irradiated with 193 nm photons resulting in asymmetric charge partitioning of subcomplexes at lower energies (0.5 to 1.5 mJ/pulse) and symmetric dissociation at higher energies (1.5 to 3.0 mJ/pulse). The ability to access both of these competing dissociation pathways is unique to UVPD and contributes to the vast array of sequence ions and enhanced sequence coverage for protein complexes not obtained by any other activation method. With its ability to generate useful sequence information, UVPD was employed to study an intrinsically disordered protein, a set of asymmetric and symmetric trimers, and three membrane protein complexes. The vast population of structures adopted by the intrinsically disordered protein, high mobility group protein AT-hook 2 (HMGA2), was characterized using UVPD and the probable binding location of two DNA hairpins was determined. Trimers in the tautomerase superfamily that have nearly identical secondary structures differ in their quaternary arrangements to form asymmetric and symmetric homooligomers. In combination with collision-induced unfolding, UVPD proved capable of differentiating the two structures owing to the preservation of noncovalent interactions in the gas phase. Aquaporin z (AqpZ), mechanosensitive channel of large conductance (MscL), and the E. coli ammonia channel (AmtB) comprise the membrane protein complexes studied herein. UVPD of these complexes resulted in unprecedented levels of characterization with backbone cleavages demonstrating no significant influence from the hydrophobicity of the residues or the mobile proton-directed cleavages, which contrasts reports using electron- and collision-based dissociation methods, respectively. UVPD has also proven effective for localizing phosphorylated residues along the C-terminal domain (CTD) of RNA polymerase II, shedding light on the CTD code that mediates transcription regulation.

Mass Spectrometry-Based Lipidomics

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Publisher : Humana
ISBN 13 : 9781071614099
Total Pages : 314 pages
Book Rating : 4.6/5 (14 download)

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Book Synopsis Mass Spectrometry-Based Lipidomics by : Fong-Fu Hsu

Download or read book Mass Spectrometry-Based Lipidomics written by Fong-Fu Hsu and published by Humana. This book was released on 2021-05-29 with total page 314 pages. Available in PDF, EPUB and Kindle. Book excerpt: This detailed volume covers conventional MS-based “shotgun lipidomics” by which samples are introduced by infusion or loop injection, as well as LC-MS-based lipidomics, which are becoming increasingly important due to the ever-increasing demand for a complete and precise lipid analysis of the complex and diversified lipids in nature. The volume features protocols applying chemical reactions, the on-line photochemical reactions combined with various MS methods for comprehensive characterization of various lipid classes, and quantification of specific and rare lipids. Written for the highly successful Methods in Molecular Biology series, chapters include introductions to their respective topics, lists of the necessary materials and reagents, step-by-step, readily reproducible laboratory protocols, and tips on troubleshooting and avoiding known pitfalls. Authoritative and practical, Mass Spectrometry-Based Lipidomics: Methods and Protocols serves as an invaluable guide for biochemists and mass spectroscopists who are interested in lipid studies.

Advanced Fragmentation Methods in Biomolecular Mass Spectrometry

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Publisher : Royal Society of Chemistry
ISBN 13 : 1839161108
Total Pages : 359 pages
Book Rating : 4.8/5 (391 download)

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Book Synopsis Advanced Fragmentation Methods in Biomolecular Mass Spectrometry by : Frederik Lermyte

Download or read book Advanced Fragmentation Methods in Biomolecular Mass Spectrometry written by Frederik Lermyte and published by Royal Society of Chemistry. This book was released on 2020-12-11 with total page 359 pages. Available in PDF, EPUB and Kindle. Book excerpt: Breaking down large biomolecules into fragments in a controlled manner is key to modern biomolecular mass spectrometry. This book is a high-level introduction, as well as a reference work for experienced users, to ECD, ETD, EDD, NETD, UVPD, SID, and other advanced fragmentation methods. It provides a comprehensive overview of their history, mechanisms, instrumentation, and key applications. With contributions from leading experts, this book will act as an authoritative guide to these methods. Aimed at postgraduate and professional researchers, mainly in academia, but also in industry, it can be used as supplementary reading for advanced students on mass spectrometry or analytical (bio)chemistry courses.

Lipidomics

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Publisher : John Wiley & Sons
ISBN 13 : 1118893123
Total Pages : 48 pages
Book Rating : 4.1/5 (188 download)

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Book Synopsis Lipidomics by : Xianlin Han

Download or read book Lipidomics written by Xianlin Han and published by John Wiley & Sons. This book was released on 2016-05-02 with total page 48 pages. Available in PDF, EPUB and Kindle. Book excerpt: Covers the area of lipidomics from fundamentals and theory to applications Presents a balanced discussion of the fundamentals, theory, experimental methods and applications of lipidomics Covers different characterizations of lipids including Glycerophospholipids; Sphingolipids; Glycerolipids and Glycolipids; and Fatty Acids and Modified Fatty Acids Includes a section on quantification of Lipids in Lipidomics such as sample preparation; factors affecting accurate quantification; and data processing and interpretation Details applications of Lipidomics Tools including for Health and Disease; Plant Lipidomics; and Lipidomics on Cellular Membranes

Tandem Mass Spectrometry of Lipids

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Publisher : Royal Society of Chemistry
ISBN 13 : 1849738270
Total Pages : 294 pages
Book Rating : 4.8/5 (497 download)

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Book Synopsis Tandem Mass Spectrometry of Lipids by : Robert C Murphy

Download or read book Tandem Mass Spectrometry of Lipids written by Robert C Murphy and published by Royal Society of Chemistry. This book was released on 2014-12-15 with total page 294 pages. Available in PDF, EPUB and Kindle. Book excerpt: The emerging field of lipidomics has been made possible because of advances in mass spectrometry, and in particular tandem mass spectrometry of lipid ions generated by electrospray ionization. The ability to carry out basic biochemical studies of lipids using electrospray ionization is predicated upon understanding the behaviour of lipid derived ions following collision induced decomposition and mechanisms of product ion formation. During the past 20 years, a wealth of information has been generated about lipid molecules that are now analysed by mass spectrometry, however there is no central source where one can obtain basic information about how these very diverse biomolecules behave following collisional activation. This book will bring together, in one volume, this information so that investigators considering using tandem mass spectrometry to structurally characterize lipids or to quantitate their occurrence in a biological matrix, will have a convenient source to review mechanism of decomposition reactions related to the diversity of lipid structures. A separate chapter is devoted to each of seven major lipid classes including fatty acids, eicosanoids and bioactive lipid mediators, fatty acyl esters and amides, glycerol esters, glycerophospholipids, sphingolipids, and steroids. Mechanistic details are provided for understanding the pathways of formation of major product ions and ions used for structural characterization. In most cases specific ancillary information has been critical to understand the pathways, including isotope labeling and high resolution analysis of precursor and product ions. For a few specific examples such data is missing and pathways are proposed as a means to initiate further mass spectral experiments to prove or disprove pathway hypotheses. While this work largely centres on the lipid biochemistry of animal (mammalian) systems, general principles can be taken from the specific examples and applied to lipid biochemistry found in plants, fungi, prokaryotes and archeal organisms.

Encyclopedia of Lipidomics

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Publisher : Springer
ISBN 13 : 9789400774667
Total Pages : 0 pages
Book Rating : 4.7/5 (746 download)

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Book Synopsis Encyclopedia of Lipidomics by : Markus R. Wenk

Download or read book Encyclopedia of Lipidomics written by Markus R. Wenk and published by Springer. This book was released on 2018-07-11 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: The Encyclopedia of Lipidomics will present a complete overview of the field from fundamentals to new discoveries and from concepts, theories and experimental techniques to clinical and industrial applications. The book will develop with the active involvement of a strong editorial board comprised of leaders from the field. The Encyclopedia of Lipidomics intends to be a comprehensive reference resource serving to bridge the gap between clinical and basic science investigators and provide authoritative and digested information to students, scientists as well as non specialists. The book will have an edge over protocol type of works and databases in terms of having wider coverage through rigorous essays on terms, concepts, experimental and analytical techniques, applications and new challenges. Since lipidomics has strong linkages with several of the other biomedical and life sciences disciplines, the proposed encyclopedia will have a wide audience including graduate students, researchers and different levels of scientists in biomedicine, cellular and molecular biology, bioengineering, physiological and biochemistry, and pharmacology across both academia and industry.

Chiral Analysis

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Publisher : Elsevier
ISBN 13 : 0080469280
Total Pages : 721 pages
Book Rating : 4.0/5 (84 download)

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Book Synopsis Chiral Analysis by : Kenneth W. Busch

Download or read book Chiral Analysis written by Kenneth W. Busch and published by Elsevier. This book was released on 2011-10-13 with total page 721 pages. Available in PDF, EPUB and Kindle. Book excerpt: Chiral Analysis covers an important area of analytical chemistry of relevance to a wide variety of scientific professionals. The target audience is scientific professionals with an undergraduate background in chemistry or a related discipline, specifically organic chemists, researchers in drug discovery, pharmaceutical researchers involved with process analysis or combinatorial libraries, and graduate students in chemistry. Chapters have been written with the nonspecialist in mind so as to be self-contained. * Broad coverage - spectroscopic and separation methods covered in a single volume * Up-to-date and detailed review of the various techniques available and/or under development in this field * Contributions from leading experts in the field

Triboelectric Nanogenerators

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Publisher : Springer
ISBN 13 : 3319400398
Total Pages : 537 pages
Book Rating : 4.3/5 (194 download)

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Book Synopsis Triboelectric Nanogenerators by : Zhong Lin Wang

Download or read book Triboelectric Nanogenerators written by Zhong Lin Wang and published by Springer. This book was released on 2016-08-17 with total page 537 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book introduces an innovative and high-efficiency technology for mechanical energy harvesting. The book covers the history and development of triboelectric nanogenerators, basic structures, working principles, performance characterization, and potential applications. It is divided into three parts: Part A illustrates the fundamental working modes of triboelectric nanogenerators with their prototype structures and theoretical analysis; Part B and Part C introduce two categories of applications, namely self-powered systems and self-powered active sensors. The book will be an ideal guide to scientists and engineers beginning to study triboelectric nanogenerators or wishing to deepen their knowledge of the field. Readers will be able to place the technical details about this technology in context, and acquire the necessary skills to reproduce the experimental setups for fabrication and measurement.

Protein Structure Analysis

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Publisher : Springer Science & Business Media
ISBN 13 : 3642592198
Total Pages : 311 pages
Book Rating : 4.6/5 (425 download)

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Book Synopsis Protein Structure Analysis by : Roza Maria Kamp

Download or read book Protein Structure Analysis written by Roza Maria Kamp and published by Springer Science & Business Media. This book was released on 2012-12-06 with total page 311 pages. Available in PDF, EPUB and Kindle. Book excerpt: "Protein Structure Analysis - Preparation and Characterization" is a compilation of practical approaches to the structural analysis of proteins and peptides. Here, about 20 authors describe and comment on techniques for sensitive protein purification and analysis. These methods are used worldwide in biochemical and biotechnical research currently being carried out in pharmaceu tical and biomedical laboratories or protein sequencing facilities. The chapters have been written by scientists with extensive ex perience in these fields, and the practical parts are well documen ted so that the reader should be able to easily reproduce the described techniques. The methods compiled in this book were demonstrated in student courses and in the EMBO Practical Course on "Microsequence Analysis of Proteins" held in Berlin September 10-15, 1995. The topics also derived from a FEBS Workshop, held in Halkidiki, Thessaloniki, Greece, in April, 1995. Most of the authors participated in these courses as lecturers and tutors and made these courses extremely lively and successful. Since polypeptides greatly vary depending on their specific structure and function, strategies for their structural analysis must for the most part be adapted to each individual protein. Therefore, advantages and limitations of the experimen tal approaches are discussed here critically, so that the reader becomes familiar with problems that might be encountered.

Lipidomics

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Publisher : John Wiley & Sons
ISBN 13 : 3527655964
Total Pages : 507 pages
Book Rating : 4.5/5 (276 download)

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Book Synopsis Lipidomics by : Kim Ekroos

Download or read book Lipidomics written by Kim Ekroos and published by John Wiley & Sons. This book was released on 2012-09-04 with total page 507 pages. Available in PDF, EPUB and Kindle. Book excerpt: Focusing on the practical applications, this user-oriented guide presents current technologies and strategies for systems-level lipid analysis, going beyond basic research to concentrate on commercial uses of lipidomics in biomarker and diagnostic development, as well as within pharmaceutical drug discovery and development. The editor and authors have experience of the most recent analytical instruments and techniques, allowing them to provide here first-hand practical experience for newcomers to the field. The first half of the book covers current methodologies, ranging from global to targeted lipidomics and shotgun approaches, while the second part discusses the role of lipidomics in biomedical and pharmaceutical research, covering such diverse fields as inflammation, metabolic syndrome, cardiovascular and neurological disease. Both small and large-scale, high-throughput approaches are discussed, resulting in an invaluable source for academic and industrial research and development.