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Bacterial Amyloids

Bacterial Amyloids
Author: Véronique Arluison
Publisher: Springer Nature
Total Pages: 336
Release: 2022-08-11
Genre: Science
ISBN: 1071625292

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This detailed volume introduces different methods to assess the structure and folding of bacterial amyloids and analyze their functions, either in vitro or in vivo. Despite their initial association with neurodegenerative diseases, there is now increasing evidence of alternative roles for amyloids, with beneficial aspects for cells. In particular, prokaryotes use amyloids as functional assemblies, where they are key players in the cell's physiology. 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 up-to-date, Bacterial Amyloids: Methods and Protocols is an ideal guide for experts and novices alike to further explore these crucial protein assemblies.


Protein Solubility and Aggregation in Bacteria

Protein Solubility and Aggregation in Bacteria
Author: Salvador Ventura
Publisher: Frontiers Media SA
Total Pages: 129
Release: 2016-09-26
Genre: Microbiology
ISBN: 2889199762

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Proteins suffer many conformational changes and interactions through their life, from their synthesis at ribosomes to their controlled degradation. Only folded and soluble proteins are functional. Thus, protein folding and solubility are controlled genetically, transcriptionally, and at the protein sequence level. In addition, a well-conserved cellular machinery assists the folding of polypeptides to avoid misfolding and ensure the attainment of soluble and functional structures. When these redundant protective strategies are overcome, misfolded proteins are recruited into aggregates. Recombinant protein production is an essential tool for the biotechnology industry and also supports expanding areas of basic and biomedical research, including structural genomics and proteomics. Although bacteria still represent a convenient production system, many recombinant polypeptides produced in prokaryotic hosts undergo irregular or incomplete folding processes that usually result in their accumulation as insoluble aggregates, narrowing thus the spectrum of protein-based drugs that are available in the biotechnology market. In fact, the solubility of bacterially produced proteins is of major concern in production processes, and many orthogonal strategies have been exploited to try to increase soluble protein yields. Importantly, contrary to the usual assumption that the bacterial aggregates formed during protein production are totally inactive, the presence of a fraction of molecules in a native-like structure in these assemblies endorse them with a certain degree of biological activity, a property that is allowing the use of bacteria as factories to produce new functional materials and catalysts. The protein embedded in intracellular bacterial deposits might display different conformations, but they are usually enriched in beta-sheet-rich assemblies resembling the amyloid fibrils characteristic of several human neurodegenerative diseases. This makes bacterial cells simple, but biologically relevant model systems to address the mechanisms behind amyloid formation and the cellular impact of protein aggregates. Interestingly, bacteria also exploit the structural principles behind amyloid formation for functional purposes such as adhesion or cytotoxicity. In the present research topic we collect papers addressing all the issues mentioned above from both the experimental and computational point of view.


Preparation and Characterization of Functional Amyloids and Amyloid-based Biofilm in Escherichia Coli

Preparation and Characterization of Functional Amyloids and Amyloid-based Biofilm in Escherichia Coli
Author: Oscar Aloysius McCrate
Publisher:
Total Pages:
Release: 2013
Genre:
ISBN:

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Amyloids are a special class of proteins possessing a common cross-beta fold. This cross-beta fold confers a number of unique properties including insolubility, resistance to thermal and chaotropic denaturation, protease resistance, and the ability to spontaneously self-template and auto-aggregate into fibers. Microorganisms have harnessed the power of the amyloid fold to produce a variety of functional amyloids. In microorganisms, amyloids are involved in many functions including: serving as non-chromosomal genetic elements in the form of prions; serving as surface modifiers in the form of hydrophobins and chaplins; and are used to form multifunctional extracellular fibrillar structures. Amyloid-based fimbriae appear to be prevalent in nature and play a huge number of roles from surface adhesive structures and virulence factors to structural components in biofilms. Curli fibers were the first bacterial functional amyloid fibers discovered. In Escherichia coli, curli are produced as extracellular surface adhesive structures mediating cell-cell interactions, binding to biotic and abiotic surfaces, and serving as major structural components in biofilm formation. The uropathogenic E. coli strain UTI89 is capable of forming a highly insoluble amyloid-mediated biofilm. Biofilms consist of bacteria plus their secreted extracellular matrix (ECM). The amyloid-mediated UTI89 ECM is known to contain curli and a polysaccharide believed to be cellulose; however, it is likely that other components are present. In this dissertation, two biological systems were developed, biochemically characterized, and analyzed by solid state NMR--(1) in vivo-assembled curli amyloid fibers and (2) the curli/cellulose-based ECM of E. coli strain UTI89. Solid state NMR was used for analysis due to its ability to provide data on both the structure and chemical composition of intact, insoluble biological assemblies. Examination of the intact biological assemblies required the use of the native bacterial expression and assembly systems. Thus high expression levels were achieved through manipulation of bacterial physiology via optimization of environmental conditions. Expression on both undefined, rich defined, and minimal defined media was optimized to enable maximum flexibility in the isotopic labeling of samples for detailed NMR studies. Minimally perturbative extractions were developed and optimized for curli and UTI89 ECM production. For both the curli and UTI89 ECM systems,> 100 mg yields are accessible. Most biochemical analyses were developed for soluble systems. Thus, the biochemical analysis of curli fibers and the UTI89 ECM required the development of new techniques and validation of pre-existing methods due to the insolubility of these systems. Additionally, new methods were developed to facilitate tracking and analysis of the curli and UTI89 ECM systems including a simple method for tracking the purification of extracellular structures using microbiological indicator dyes and an apparatus to simulate growth on agar using track-etched membranes and broth. Initial solid state NMR characterization of both the curli and UTI89 ECM systems were carried out. Isotopic labels were selectively incorporated into curli and the label incorporation was characterized. For the UTI89 ECM system, the ECM composition was examined and quantified by solid state NMR. It was found that the polysaccharide portion of the UTI89 ECM is a modified form of cellulose, and that the composition of our purified ECM is approximately 85% curli and 15% modified cellulose. Taken as a whole, the work presented in this thesis is an excellent beginning. The systems developed are naturally expressed, natively assembled, and biologically relevant yet are still robust and high yielding. Because these systems were optimized for solid state NMR, ample material is available for any other conceivable biochemical or biophysical assay. Basic characterization of these systems has been performed laying the foundation for more detailed future studies. Additionally, the indicator dye tracking and ECM purification tools have been found to be easily implementable and applicable to other biofilm systems thereby driving exploration and innovation.


Amyloid Fibrils and Prefibrillar Aggregates

Amyloid Fibrils and Prefibrillar Aggregates
Author: Daniel Erik Otzen
Publisher: John Wiley & Sons
Total Pages: 496
Release: 2013-06-04
Genre: Science
ISBN: 3527654208

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Summing up almost a decade of biomedical research, this topical and eagerly awaited handbook is the first reference on the topic to incorporate recent breakthroughs in amyloid research. The first part covers the structural biology of amyloid fibrils and pre-fibrillar assemblies, including a description of current models for amyloid formation. The second part looks at the diagnosis and biomedical study of amyloid in humans and in animal models, while the final section discusses pharmacological approaches to manipulating amyloid and also looks at its physiological roles in lower and higher organisms. For Biochemists, Molecular Biologists, Neurobiologists, Neurophysiologists and those working in the Pharmaceutical Industry.


Peptide Catalysts, including Catalytic Amyloids

Peptide Catalysts, including Catalytic Amyloids
Author:
Publisher: Elsevier
Total Pages: 550
Release: 2024-05-28
Genre: Science
ISBN: 0443236682

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Peptide Catalysts, including Catalytic Amyloids, Volume 697 in this esteemed series, highlights new advances in the field, with this new volume presenting interesting topics on Screening of oxidative behaviors in catalytic amyloid assemblies, Catalytic amyloids derived for natural proteins, AFM-IR studies of catalytic amyloids, MD structural studies of catalytic amyloids, Characterization of crystalline, amyloid-like amino acid assemblies, Computational modeling of supramolecular peptide assemblies, and Assembly and activity of short prion-inspired peptides. Provides the authority and expertise of leading contributors from an international board of authors Presents the latest release in Methods in Enzymology series Updated release includes the latest information on Peptide Catalysts, including Catalytic Amyloids


Alzheimer's Disease

Alzheimer's Disease
Author: Thimmaiah Govindaraju
Publisher: Royal Society of Chemistry
Total Pages: 531
Release: 2022-01-04
Genre: Medical
ISBN: 1839162740

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Alzheimer’s disease is an increasingly common form of dementia and despite rising interest in discovery of novel treatments and investigation into aetiology, there are no currently approved treatments that directly tackle the causes of the condition. Due to its multifactorial pathogenesis, current treatments are directed against symptoms and even precise diagnosis remains difficult as the majority of cases are diagnosed symptomatically and usually confirmed only by autopsy. Alzheimer’s Disease: Recent Findings in Pathophysiology, Diagnostic and Therapeutic Modalities provides a comprehensive overview from aetiology and neurochemistry to diagnosis, evaluation and management of Alzheimer's disease, and latest therapeutic approaches. Intended to provide an introduction to all aspects of the disease and latest developments, this book is ideal for students, postgraduates and researchers in neurochemistry, neurological drug discovery and Alzheimer’s disease.


Immune Response to Biofilms

Immune Response to Biofilms
Author: Semih Esin
Publisher: Frontiers Media SA
Total Pages: 134
Release: 2021-08-02
Genre: Medical
ISBN: 2889711331

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Human Hemostasis

Human Hemostasis
Author: American Association of Blood Banks
Publisher: American Association of Blood Banks (AABB)
Total Pages: 74
Release: 1975-12
Genre: Medical
ISBN: 9780914404217

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