Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A

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ISBN 13 :
Total Pages : 20 pages
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Book Synopsis Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A by : Nicole Appel

Download or read book Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A written by Nicole Appel and published by . This book was released on 2004 with total page 20 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A.

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Book Synopsis Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A. by :

Download or read book Structural and Functional Analysis of the Hepatitis C Virus Non-structural Protein 5A. written by and published by . This book was released on 2004 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: Das Hepatitis C Virus (HCV) ist ein umhülltes RNA Virus aus der Familie der Flaviviridae. Sein Genom kodiert für ein ca. 3000 Aminosäuren langes Polyprotein, welches co- und posttranslational in seine funktionellen Einheiten gespalten wird. Eines dieser viralen Proteine ist NS5A. Es handelt sich hierbei um ein stark phosphoryliertes Protein, das eine amphipatische α-Helix im Amino-Terminus trägt, welche für die Membran-Assoziation von NS5A verantwortlich ist. Welche Rolle die Phosphorylierung für die Funktion des Proteins spielt, bzw. welche Funktion NS5A überhaupt ausübt, ist zur Zeit noch unklar. Beobachtungen lassen Vermutungen über eine Funktion von NS5A bei der Resistenz infizierter Zellen gegenüber Interferon-alpha zu. Weiterhin wird vermutet, das NS5A als Komponente des membranständigen HCV Replikasekomplexes an der RNA Replikation beteiligt ist. Das Ziel dieser Doktorarbeit war es, die Funktion von NS5A für die RNA Replikation zu untersuchen. Zu diesem Zweck wurde eine Serie von Phosphorylierungsstellen-Mutanten generiert, die auf Ihre Replikationsfähigkeit und den Phosphorylierungsstatus hin untersucht wurden. Wir fanden, dass bestimmte Serin-Substitutionen im Zentrum von NS5A zu einer gesteigerten RNA Replikation führten, bei gleichzeitig reduzierter NS5A Hyperphosphorylierung. Weiterhin studierten wir den Einfluß von Mutationen in der Amino-terminalen amphipatischen α-Helix von NS5A auf die RNA-Replikation, sowie Phosphorylierung und subzelluläre Lokalisation des Proteins. Wir fanden, dass geringfügige strukturelle Veränderungen der amphipatischen Helix zu einer veränderten subzellulären Lokalisation von NS5A führten, was mit einer reduzierten oder komplett inhibierten RNA Replikation einherging. Zudem interferierten die strukturellen Veränderungen mit der Hyperphosphorylierung des Proteins, was den Schluß nahe legt, dass die amphipatische Helix eine wichtige strukturelle Komponente des Proteins darstellt, die für die korrekte Faltung und Phosphorylierung.

Functional Analysis of Domain I of the Hepatitis C Virus Non-structural NS5A Protein

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Total Pages : 230 pages
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Book Synopsis Functional Analysis of Domain I of the Hepatitis C Virus Non-structural NS5A Protein by : Chunhong Yin

Download or read book Functional Analysis of Domain I of the Hepatitis C Virus Non-structural NS5A Protein written by Chunhong Yin and published by . This book was released on 2018 with total page 230 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Functional Analysis of Hepatitis C Virus Non-structural Protein (NS) 3 Protease and Viral Cofactor NS4A.

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Book Synopsis Functional Analysis of Hepatitis C Virus Non-structural Protein (NS) 3 Protease and Viral Cofactor NS4A. by :

Download or read book Functional Analysis of Hepatitis C Virus Non-structural Protein (NS) 3 Protease and Viral Cofactor NS4A. written by and published by . This book was released on 2008 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: The hepatitis C virus (HCV) was identified in 1989 as the major causative agent of transfusion-associated non-A, non-B hepatitis and today represents a worldwide health crisis with prevalence estimates of 2.2%. HCV-specific therapeutics have never been more urgently needed. One of the validated drug targets is the non-structural (NS) protein 3 (NS3) membrane-bound protease. The major aim of this thesis was characterization of NS3 allosteric activation by its viral cofactor, NS4A. We hypothesized that there would be specific residues that dominate the interaction between NS3 and NS4A, and further hypothesized that binding and activation may be separate events mediated by different residues. This thesis details the development of novel cell-based assays for detection of NS3-4A protease activity and heterocomplex formation. The protease assay substrate was a membrane-targeted intracellular protein, which upon proteolysis released a red fluorescent protein (FP) reporter, DsRed-Express, into the cytoplasm; this change was detected by microscopy or quantified by Western blotting. The complex formation assay detected fluorescence resonance energy transfer (FRET) between yellow and cyan FP-tagged NS3 and NS4A, respectively. Our data shows binding can be functionally separated from activation. We identified two NS4A residues (I25 and I29) important for NS3 binding and two NS4A residues (V23 and I25) important for NS3 activation. Therefore the binding-pockets of these residues are prime targets for small-molecule therapeutic development. In addition, I have compared the NS3-4A substrate sequence cleavage efficiencies in vivo. I have been able to show that the activation-dependent NS4B/NS5A junction is processed efficiently and the NS4A/NS4B junction is not. I have also shown NS3-4A substrate specificity is not modulated by replicase components; however the specific activity of this enzyme is increased. The strength of this thesis work stems from the novel and creative develop.

Functional Characterization of Hepatitis C Virus Non-structural Protein 4B and Viral Replication Factories

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ISBN 13 :
Total Pages : 188 pages
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Book Synopsis Functional Characterization of Hepatitis C Virus Non-structural Protein 4B and Viral Replication Factories by : David Paul

Download or read book Functional Characterization of Hepatitis C Virus Non-structural Protein 4B and Viral Replication Factories written by David Paul and published by . This book was released on 2013 with total page 188 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Functional Dissection of the Hepatitis C Virus Non-structural Proteins and MiR-122 in Viral Replication and Translation

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Book Synopsis Functional Dissection of the Hepatitis C Virus Non-structural Proteins and MiR-122 in Viral Replication and Translation by : Philipp Schult

Download or read book Functional Dissection of the Hepatitis C Virus Non-structural Proteins and MiR-122 in Viral Replication and Translation written by Philipp Schult and published by . This book was released on 2016 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Role of Non-structural Protein 5A in Hepatitis C Virus Particle Production

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Total Pages : 276 pages
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Book Synopsis Role of Non-structural Protein 5A in Hepatitis C Virus Particle Production by : Margarita Laura Zayas López

Download or read book Role of Non-structural Protein 5A in Hepatitis C Virus Particle Production written by Margarita Laura Zayas López and published by . This book was released on 2010 with total page 276 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Identification of Cellular Targets of Hepatitis C Virus Non-structural Protein 5A

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ISBN 13 :
Total Pages : 133 pages
Book Rating : 4.:/5 (723 download)

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Book Synopsis Identification of Cellular Targets of Hepatitis C Virus Non-structural Protein 5A by : Tilmann Bürckstümmer

Download or read book Identification of Cellular Targets of Hepatitis C Virus Non-structural Protein 5A written by Tilmann Bürckstümmer and published by . This book was released on 2005 with total page 133 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Identification and Functional Studies of a Novel Nonstructural Protein 5A Phosphorylation Site in Hepatitis C Virus

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Book Synopsis Identification and Functional Studies of a Novel Nonstructural Protein 5A Phosphorylation Site in Hepatitis C Virus by : 鍾穎文

Download or read book Identification and Functional Studies of a Novel Nonstructural Protein 5A Phosphorylation Site in Hepatitis C Virus written by 鍾穎文 and published by . This book was released on 2012 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

The Coronaviridae

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Publisher : Springer Science & Business Media
ISBN 13 : 1489915311
Total Pages : 424 pages
Book Rating : 4.4/5 (899 download)

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Book Synopsis The Coronaviridae by : Stuart G. Siddell

Download or read book The Coronaviridae written by Stuart G. Siddell and published by Springer Science & Business Media. This book was released on 2013-06-29 with total page 424 pages. Available in PDF, EPUB and Kindle. Book excerpt: Coronaviruses were recognized as a group of enveloped, RNA viruses in 1968 and accepted by the International Committee on the Taxonomy of Viruses as a separate family, the Coronaviridae, in 1975. By 1978, it had become evident that the coronavirus genomic RNA was infectious (i. e. , positive strand), and by 1983, at least the framework of the coronavirus replication strategy had been per ceived. Subsequently, with the application of recombinant DNA techniques, there have been remarkable advances in our understanding of the molecular biology of coronaviruses, and a mass of structural data concerning coronavirus genomes, mRNAs, and pro teins now exists. More recently, attention has been focused on the role of essential and accessory gene products in the coronavirus replication cyde and a molecular analysis of the structure-function relation ships of coronavirus proteins. Nevertheless, there are still large gaps in our knowledge, for instance, in areas such as the genesis of coronavirus subgenomic mRNAs or the function of the coronavirus RNA-dependent RNA polymerase. The diseases caused by coronaviruses have been known for much longer than the agents themselves. Possibly the first coronavirus-related disease to be recorded was feline infectious peritonitis, as early as 1912. The diseases associ ated with infectious bronchitis virus, transmissible gastroenteritis virus, and murine hepatitis virus were all well known before 1950.

Functional Analysis of Viral Nonstructural and Structural Proteins

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Total Pages : 360 pages
Book Rating : 4.:/5 (437 download)

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Book Synopsis Functional Analysis of Viral Nonstructural and Structural Proteins by : Young Shin Lim Hahn

Download or read book Functional Analysis of Viral Nonstructural and Structural Proteins written by Young Shin Lim Hahn and published by . This book was released on 1989 with total page 360 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Protein-protein Interactions of the Unstructured Domain II of Hepatitis C Virus NS5A

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ISBN 13 :
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Book Synopsis Protein-protein Interactions of the Unstructured Domain II of Hepatitis C Virus NS5A by : Marianne Ngure

Download or read book Protein-protein Interactions of the Unstructured Domain II of Hepatitis C Virus NS5A written by Marianne Ngure and published by . This book was released on 2017 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: "The hepatitis C virus (HCV) non-structural 5A (NS5A) protein is a multi-functional, RNA binding protein and an essential component of the HCV replication complex. It is subdivided into 3 domains; a highly structured domain I (DI), while DII and DIII are intrinsically unstructured yet mediate crucial interactions with several viral and cellular host factors. NS5A-DII protein mediates the interaction with Cyclophilin A (CypA), a cellular cis/trans isomerase essential for viral replication. Cyclosporine A (CsA), an inhibitor of CypA, inhibits this interaction and suppresses HCV replication. Mutations that confer resistance to CsA and derivatives have been identified within NS5A-DII (D320E and Y321N in Con 1b). These mutations revive HCV replication in vivo, but the underlying mechanism for resistance remains elusive. Using a Förster Resonance Energy Transfer (FRET)-based approach, we determined a slower rate of dissociation of the resistant NS5A-DII complex with CypA, in the presence of CsA. The slow complex dissociation directly correlated with the increasing level of resistance conferred by either single or double mutations within NS5A-DII. By prolonging the protein-protein complex, D320E and Y321N specifically limit the inhibitory effect of CsA on the NS5A-DII complex with CypA, providing a possible biochemical mechanism of resistance to CypA inhibitors. Apart from its CypA binding properties, NS5A-DII also binds RNA, and interacts with the HCV RNA-dependent RNA polymerase NS5B. However, the largely disordered nature of NS5A-DII has limited the characterization of the structure and functional relevance of these interactions. A mass spectrometry (MS)-assisted foot-printing approach provided an in-depth biochemical characterization of the molecular determinants of protein-protein and nucleoprotein interactions of HCV NS5A-DII with CypA, NS5B and RNA. Overlapping but definitive binding sites for each of the three macromolecules were determined. The conserved residue W316 was identified as a principle mediator of protein-protein interaction (CypA and NS5B) while an arginine-rich region of NS5A-DII was crucial for RNA binding. Specifically, NS5A-DII K308 residue was indispensable for RNA-binding. A novel binding site of NS5A-DII on the NS5B polymerase was mapped predominantly to a region associated with RNA binding. Additionally, binding of NS5A-DII diminished the RNA binding and RNA synthesis activity of NS5B polymerase. This implies a potential regulatory function of NS5A-DII on NS5B polymerase activity. Taken together, this work pinpoints key residues in the intrinsically disordered NS5A-DII that necessitate specific viral and host interactions. NS5A-DII has been plucked from obscurity as we begin to understand the biochemical functional relevance for these interactions, and their significance to HCV replication." --

Structural and Functional Analysis of the Hepatitis C Virus P7 Ion Channel

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Book Synopsis Structural and Functional Analysis of the Hepatitis C Virus P7 Ion Channel by : Thomas F. A. Whitfield

Download or read book Structural and Functional Analysis of the Hepatitis C Virus P7 Ion Channel written by Thomas F. A. Whitfield and published by . This book was released on 2008 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Identification of a Predominant Phosphorylation Site in Non-structural Protein 5A Involved in Hepatitis C Virus Life Cycle

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Book Synopsis Identification of a Predominant Phosphorylation Site in Non-structural Protein 5A Involved in Hepatitis C Virus Life Cycle by : 高維霆

Download or read book Identification of a Predominant Phosphorylation Site in Non-structural Protein 5A Involved in Hepatitis C Virus Life Cycle written by 高維霆 and published by . This book was released on 2014 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Functional Interactions of Structural and NS Proteins of Hepatitis C Virus

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ISBN 13 :
Total Pages : 362 pages
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Book Synopsis Functional Interactions of Structural and NS Proteins of Hepatitis C Virus by : Hamed Gouklani

Download or read book Functional Interactions of Structural and NS Proteins of Hepatitis C Virus written by Hamed Gouklani and published by . This book was released on 2011 with total page 362 pages. Available in PDF, EPUB and Kindle. Book excerpt: Hepatitis C virus (HCV) is a small enveloped virus with a positive-sense single stranded RNA genome. Based on its molecular genetic characteristics, the virus has been classified into the Hepacivirus genus of the family Flaviviridae. HCV is one of the major causes of chronic hepatitis which can lead to liver cirrhosis and hepatocellular carcinoma. According to the recent WHO published data, 123 million individuals are infected with HCV (approximately 3% of the world's population) throughout the world. Due to its highly variable nature, HCV is classified into six major genotypes. The HCV genome encodes a single polyprotein that is cleaved to yield at least 10 mature proteins (C, E1, E2, p7, NS2, NS3, NS4A, NS4B, NS5A and NS5B). The recently developed HCV cell culture system, based on the JFH1 strain of HCV, has provided an opportunity to study the role of the viral proteins in the complete HCV replication cycle in human hepatoma cells. How the viral proteins functionally interact during replication of HCV in cell culture is not completely understood. Passage of cell cultures transfected with HCV genomic RNA containing attenuating mutations allows for the selection of genomes with second site compensatory mutations that restore replication to wild type levels. Using this approach, the functional interactions of p7 and E2 with other viral proteins during HCV replication was investigated.A small protein of 63 amino acids, p7 is encoded at the junction of the structural and non-strucutural region. p7 is a highly hydrophobic, integral membrane protein and is classified in the viroporin family. In this thesis, it is shown that p7 is critical for production of viral particles and is implicated in a late step of particle assembly. Since the protein plays a critical role in the virus life cycle, chemical compounds that block p7 function are potential candidates for anti-viral therapy. In this thesis, a chimeric JFH1 genome that encodes the p7 protein of genotype (GT) 1b strain J4 was generated. The intergenotypic chimeric genome was nonviable in human hepatoma cells and infectious chimeric virions were only produced after cells harboring the chimeric genomes were passaged several times. To investigate the emergence of compensatory mutations in the viral proteins during cell passaging, the consensus sequences of the entire polyprotein coding regions of the wild type JFH1 and three chimeric viruses were determined. Sequence analysis revealed mutations in core, NS2, NS5A and NS5B. Reverse genetic analysis demonstrated that any one of the single mutations restored the infectivity of the defective chimeric genomes. These data suggest that there are critical genetic interactions between p7 with core, NS2, NS5A and NS5B. In addition, a stable physical interaction between p7 and NS2 is shown in a transient expression system. The HCV glycoproteins E1 and E2 are present on the surface of virions as a heterodimer that attach virions to host cell receptors and facilitate virus fusion and entry. HCV entry proceeds via attachment to glycosaminoglycans followed by binding to scavenger receptor type B class I, and the tetraspanin CD81. Recently, claudin-1 and occludin have emerged as additional receptors required for entry. E2 has a receptor binding domain (E2661RBD) that conatins three variable regions, hypervariable regions 1 (HVR1), HVR2 and the intergenotypic variable region (igVR). In this thesis, HVR1 of E2 was deleted in the context of full-length replication comptetent HCV. Deletion of HVR1 increases CD81-binding ability of the mutant and also increases its susceptibility to neutralizing antibody MAb 24. The infectivity of the HVR1 deleted virions was attenuated approximately 10-fold prior to accumulation of compensatory mutations. Sequencing of cDNA obtained from reverted virions revealed mutations in E1 (I262L) and E2 (N415D). Reverse genetic studies revealed that I262L improved the infectivity of HVR1 deleted virions 2.5 fold while N415D restored infectivity to wild type levels. These data suggest that mutations within E1 or E2 can compensate for the reduction in infectivity observed for HVR1 deleted viruses.In summary, this thesis demonstrates the importance of functional interactions between HCV proteins during virus morphogenesis and infectivity.

Studies on the hyperphosphorylation of hepatitis C virus non structural protein NS5A

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ISBN 13 :
Total Pages : 246 pages
Book Rating : 4.:/5 (111 download)

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Book Synopsis Studies on the hyperphosphorylation of hepatitis C virus non structural protein NS5A by : Michela Marongiu

Download or read book Studies on the hyperphosphorylation of hepatitis C virus non structural protein NS5A written by Michela Marongiu and published by . This book was released on 2009 with total page 246 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Structural and Functional Analysis of CD81-Claudin-1, a Hepatitis C Virus Receptor Complex

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Book Synopsis Structural and Functional Analysis of CD81-Claudin-1, a Hepatitis C Virus Receptor Complex by : Michelle Clare

Download or read book Structural and Functional Analysis of CD81-Claudin-1, a Hepatitis C Virus Receptor Complex written by Michelle Clare and published by . This book was released on 2015 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: