15 research outputs found

    Recent advances in marburgvirus research [version 1; peer review: 3 approved]

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    Marburgviruses are closely related to ebolaviruses and cause a devastating disease in humans. In 2012, we published a comprehensive review of the first 45 years of research on marburgviruses and the disease they cause, ranging from molecular biology to ecology. Spurred in part by the deadly Ebola virus outbreak in West Africa in 2013–2016, research on all filoviruses has intensified. Not meant as an introduction to marburgviruses, this article instead provides a synopsis of recent progress in marburgvirus research with a particular focus on molecular biology, advances in animal modeling, and the use of Egyptian fruit bats in infection experiments

    Investigations of Cell-Penetrating and Membrane-Pore Forming Peptides

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    Cell-penetrating and membrane-pore forming peptides are a class of membrane-active peptides. They are short sequence peptides having both hydrophilic and lipophilic combinations of amino acids. These peptides can have contrast functional diversity. Peptides encoded by viruses function as viroporins and play a critical role in viral replication, propagation, and pathogenesis. One such peptide is the Ebola virus delta peptide, which forms a pore in the host cell membrane. Another set of pore-forming peptides are antimicrobial Lantibiotic peptides that may be useful for killing antibiotic resistant bacteria by disrupting the bacterial membrane through two different possible mechanisms. Not only can they form pores that disrupt the bacterial membrane, Lantibiotics can also hinder the function of a bacterial membrane molecule, Lipid II, that is essential for cell wall biosynthesis. I performed Molecular Dynamics (MD) simulation to investigate the membrane pore-forming mechanism of the Ebola virus delta peptide. I found that the Ebola virus delta peptide forms a pentameric pore in the host cell membrane. The pore is selective for negatively charged ions, and the disulfide link between Cysteine 29 and 38 is essential for stable and effective membrane-pore formation. Similarly, I studied Lipid II binding and membrane-pore forming activity of several Lantibiotics: Nisin, Mutacin 1140, Gallidermin, NAI107, and NVB302. The computational results from MD simulations show that Nisin forms the most effective water channel in the bacterial membrane, but Gallidermin has the best Lipid II binding profile. Mutacin 1140 also binds strongly with Lipid II and forms an efficient water channel in the bacterial membrane. I also performed MD computations on a variety of mutated peptides of Mutacin 1140 and the Ebola virus delta peptides and investigated their water solubility, Lipid II binding, and membrane insertion profile. These results provide insight into the possible antimicrobial peptides with an optimized drug profile

    Emerging Diversity in Lipid-Protein Interactions

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    Membrane lipids interact with proteins in a variety of ways, ranging from providing a stable membrane environment for proteins to being embedded in to detailed roles in complicated and well-regulated protein functions. Experimental and computational advances are converging in a rapidly expanding research area of lipid-protein interactions. Experimentally, the database of high-resolution membrane protein structures is growing, as are capabilities to identify the complex lipid composition of different membranes, to probe the challenging time and length scales of lipid-protein interactions, and to link lipid-protein interactions to protein function in a variety of proteins. Computationally, more accurate membrane models and more powerful computers now enable a detailed look at lipid-protein interactions and increasing overlap with experimental observations for validation and joint interpretation of simulation and experiment. Here we review papers that use computational approaches to study detailed lipid-protein interactions, together with brief experimental and physiological contexts, aiming at comprehensive coverage of simulation papers in the last five years. Overall, a complex picture of lipid-protein interactions emerges, through a range of mechanisms including modulation of the physical properties of the lipid environment, detailed chemical interactions between lipids and proteins, and key functional roles of very specific lipids binding to well-defined binding sites on proteins. Computationally, despite important limitations, molecular dynamics simulations with current computer power and theoretical models are now in an excellent position to answer detailed questions about lipid-protein interactions

    Streptococcal collagen-like protein 1, Scl1, modulates group a Streptococcus adhesion, biofilm formation and virulence

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    Background: The collagens comprise a large family of versatile proteins found in all three domains of life. The streptococcal collagen-like protein 1, scl1, of group A Streptococcus (GAS) binds extracellular matrix components (ECM), cellular fibronectin and laminin, via the surface-exposed globular domain. GAS strains express scl1 and form biofilm in vitro, except for M3-type strains that are particularly invasive to humans. Hypothesis: Lack of scl1 adhesin in M3 GAS results in decreased adherence and biofilm formation, and increased virulence. Results and Discussion : First crystal structure of the globular domain revealed a unique six-helical bundle fold, consisting of three pairs of alpha helices connected by variable loops. ECM binding by Scl1 promotes the formation of stable tissue microcolonies, which was demonstrated in vitro during infection of wounded human skin equivalents. A conserved nonsense mutation was identified in the scl1 allele of the M3-type strains (scl1.3) that truncates the coding sequence, presumably resulting in a secreted Scl1 variant. Absence of Scl1 on the surface of M3-type GAS was demonstrated experimentally, as well as diminished expression of the scl1 transcript in M3 strains relative to other M-types. Therefore, M3-type strains have reduced biofilm capacity on ECM coatings relative to other M-types. Constructed full-length recombinant Scl1.3 protein displayed binding capacity to cellular fibronectin and laminin, and M3 strains complemented with functional Scl1.3 adhesin displayed increased biofilm formation. The isoallelic M3 strain, carrying a rare carrier allele encoding cell-associated Scl1.3 variant, showed decreased pathology in mice, compared to the invasive M3 strain. Similarly, scl1 inactivation in biofilm-capable M28- and M41-type GAS led to increased lesion size during subcutaneous infection. Conclusions: The studies presented here demonstrate the importance of surface Scl1 in modulating biofilm formation and virulence of GAS, and provide insight into the structure and function of Scl proteins

    MC 2019 Berlin Microscopy Conference - Abstracts

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    Das Dokument enthält die Kurzfassungen der Beiträge aller Teilnehmer an der Mikroskopiekonferenz "MC 2019", die vom 01. bis 05.09.2019, in Berlin stattfand

    Going viral : an integrated view on virological data analysis from basic research to clinical applications

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    Viruses are of considerable interest for several fields of life science research. The genomic richness of these entities, their environmen- tal abundance, as well as their high adaptability and, potentially, pathogenicity make treatment of viral diseases challenging. This thesis proposes three novel contributions to antiviral research that each concern analysis procedures of high-throughput experimen- tal genomics data. First, a sensitive approach for detecting viral genomes and transcripts in sequencing data of human cancers is presented that improves upon prior approaches by allowing de- tection of viral nucleotide sequences that consist of human-viral homologs or are diverged from known reference sequences. Sec- ond, a computational method for inferring physical protein contacts from experimental protein complex purification assays is put for- ward that allows statistically meaningful integration of multiple data sets and is able to infer protein contacts of transiently binding protein classes such as kinases and molecular chaperones. Third, an investigation of minute changes in viral genomic populations upon treatment of patients with the mutagen ribavirin is presented that first characterizes the mutagenic effect of this drug on the hepatitis C virus based on deep sequencing data.Viren sind von beträchtlichem Interesse für die biowissenschaftliche Forschung. Der genetische Reichtum, die hohe Vielfalt, wie auch die Anpassungsfähigkeit und mögliche Pathogenität dieser Organismen erschwert die Behandlung von viralen Erkrankungen. Diese Promotionsschrift enthält drei neuartige Beiträge zur antiviralen Forschung welche die Analyse von experimentellen Hochdurchsatzdaten der Genomik betreffen: erstens, ein sensitiver Ansatz zur Entdeckung viraler Genome und Transkripte in Sequenzdaten humaner Karzinome, der die Identifikation von viralen Nukleotidsequenzen ermöglicht, die von Referenzgenomen ab- weichen oder homolog zu humanen Faktoren sind. Zweitens, eine computergestützte Methode um physische Proteinkontakte von experimentellen Proteinkomplex-Purifikationsdaten abzuleiten welche die statistische Integration von mehreren Datensätzen erlaubt um insbesondere Proteinkontakte von flüchtig interagierenden Proteinklassen wie etwa Kinasen und Chaperonen aus den Daten ableiten zu können. Drittens, eine Untersuchung von kleinsten Änderungen viraler Genompopulationen während der Behandlung von Patienten mit dem Mutagen ribavirin die zum ersten Mal die mutagene Wirkung dieses Medikaments auf das Hepatitis C Virus mittels Tiefensequenzdaten nachweist
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