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2. Neue Ansätze zur Hemmung der HIV-Replikation

Author

Rebensburg, S.

Abstract

Das größte Problem für HIV-infizierte Personen ist die Tatsache, dass die Infektion nicht „geheilt“ werden kann und die Betroffenen ihr Leben lang infiziert bleiben. Deshalb erfordert die HIV Infektion die dauerhafte Anwendung von Therapien, die das Virus an der Replikation hindern und damit die „Viruslast“ im Körper möglichst gering halten. Die optimale Bekämpfung der HIV-Infektion wären Wirkstoffkombinationen die sowohl die Produktion des Virus durch persistent infizierte Reservoirs als auch die Neuinfektion von HIV-Zielzellen unterbinden. Interessanterweise sind einige zelluläre Faktoren bekannt, die in die HIV-Replikation eingreifen und der HIV-Produktion entgegenwirken können. Ein Beispiel für solche HIV-Restriktionsfaktoren sind die Risp/ Fam21 Proteine, die mit dem HIV Rev Protein interagieren und so vermutlich seine regulatorische Funktion hemmen können. Frühere Untersuchungen an persistent HIV-infizierten Astrozyten belegten einen Zusammenhang zwischen der Expressionsstärke von Risp/ Fam21 und der Hemmung der HIV Produktion in diesen Zellen. In dieser Arbeit wurde mit Hilfe der quantitativen PCR Analyse gezeigt, dass risp/ fam21 Gene in unterschiedlichen Stärken in menschlichen Zellen exprimiert werden. Zur Modulation der Risp/ Fam21 Expression in diesen als auch anderen für HIV relevanten Zellen wurde ein lentivirales Vektorsystem etabliert. In akut infizierten T-Zellen wurde kein Einfluss der Risp/ Fam21-Modulation auf die HIV-Infektion gefunden, was die Theorie nahelegt, dass Risp/ Fam21 Proteine nur in persistent infizierten Zellen wie den o.g. Astrozyten eine Aktivität zeigen könnten. Um neue Inhibitoren der akuten HIV-Infektion gesunder Zellen zu identifizieren, wurde die medizinische Heilpflanze Cistus incanus (Ci) im Hinblick auf ihre anti-HIV Aktivität getestet. Bei dieser Pflanze handelt es sich um eine sehr polyphenolreiche Pflanze und Polyphenole stellen eine interessante Klasse an HIV-Inhibitoren dar. In der vorliegenden Arbeit wurde gezeigt, dass Präparate aus Ci die Infektion von Zellen hemmen, indem sie spezifisch an die Virusoberfläche binden und die Anheftung der Viren an die Zielzellen verhindern. Präparate aus Ci inhibieren ein sehr breites Spektrum an verschiedenen HIV-Laborstämmen und –Patientenisolaten.

Published
2015

6. T cells with low CD2 levels express reduced restriction factors and are preferentially infected in therapy naïve chronic HIV-1 patients.

Author

Bolduan S, Koppensteiner H, Businger R, Rebensburg S, Kunze C, Brack-Werner R, Draenert R, and Schindler M

Subjects
Adult, Aged, Female, HIV Infections virology, Humans, Leukocytes, Mononuclear immunology, Leukocytes, Mononuclear virology, Male, Middle Aged, SAM Domain and HD Domain-Containing Protein 1 genetics, SAM Domain and HD Domain-Containing Protein 1 immunology, T-Lymphocytes virology, Viral Load, HIV Infections genetics, HIV Infections immunology, HIV-1 physiology, T-Lymphocytes immunology
Abstract

Introduction: Restriction factors (RFs) suppress HIV-1 in cell lines and primary cell models. Hence, RFs might be attractive targets for novel antiviral strategies, but their importance for virus control in vivo is controversial., Methods: We profiled the expression of RFs in primary blood-derived mononuclear cells (PBMC) from therapy-naïve HIV-1 patients and quantified infection., Results: Overall, there was no correlation between individual RF expression and HIV-1 status in total PBMC. However, we identified a T cell population with low levels of intracellular CD2 and reduced expression of SAMHD1, p21 and SerinC5. CD2 low T cells with reduced RF expression were markedly positive for HIV-1 p24. In contrast, CD2+ T cells were less infected and expressed higher levels of RFs. CD2 low T cell infection correlated with viral loads and was associated with HIV-1 disease progression., Conclusions: In untreated therapy naïve chronic HIV-1 patients, RF expression in T cells is associated with CD2 expression and seems to influence viral loads. Our study suggests that RFs help to control HIV-1 infection in certain T cells in vivo and supports the potential for RFs as promising targets for therapeutic intervention., Competing Interests: The authors declare that they have no competing interests.

Published
2017
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7. HIV-1 Integrase Binds the Viral RNA Genome and Is Essential during Virion Morphogenesis.

Author

Kessl JJ, Kutluay SB, Townsend D, Rebensburg S, Slaughter A, Larue RC, Shkriabai N, Bakouche N, Fuchs JR, Bieniasz PD, and Kvaratskhelia M

Subjects
HEK293 Cells, HIV Integrase genetics, HIV Integrase Inhibitors pharmacology, HIV-1 drug effects, HIV-1 enzymology, Humans, Morphogenesis, Nucleocapsid drug effects, Protein Binding, Virion drug effects, Virion enzymology, Virus Integration drug effects, Genome, Viral, HIV Integrase metabolism, HIV-1 growth & development, RNA, Viral metabolism, Virion growth & development
Abstract

While an essential role of HIV-1 integrase (IN) for integration of viral cDNA into human chromosome is established, studies with IN mutants and allosteric IN inhibitors (ALLINIs) have suggested that IN can also influence viral particle maturation. However, it has remained enigmatic as to how IN contributes to virion morphogenesis. Here, we demonstrate that IN directly binds the viral RNA genome in virions. These interactions have specificity, as IN exhibits distinct preference for select viral RNA structural elements. We show that IN substitutions that selectively impair its binding to viral RNA result in eccentric, non-infectious virions without affecting nucleocapsid-RNA interactions. Likewise, ALLINIs impair IN binding to viral RNA in virions of wild-type, but not escape mutant, virus. These results reveal an unexpected biological role of IN binding to the viral RNA genome during virion morphogenesis and elucidate the mode of action of ALLINIs., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published
2016
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8. Potent in vitro antiviral activity of Cistus incanus extract against HIV and Filoviruses targets viral envelope proteins.

Author

Rebensburg S, Helfer M, Schneider M, Koppensteiner H, Eberle J, Schindler M, Gürtler L, and Brack-Werner R

Subjects
Antiviral Agents chemistry, Cell Line, Cells, Cultured, Dose-Response Relationship, Drug, Drug Resistance, Viral, Humans, Microbial Sensitivity Tests, Plant Extracts chemistry, Polyphenols chemistry, Polyphenols pharmacology, Virus Replication drug effects, Antiviral Agents pharmacology, Cistus chemistry, Filoviridae drug effects, HIV-1 drug effects, Plant Extracts pharmacology, Viral Envelope Proteins antagonists & inhibitors
Abstract

Novel therapeutic options are urgently needed to improve global treatment of virus infections. Herbal products with confirmed clinical safety features are attractive starting material for the identification of new antiviral activities. Here we demonstrate that Cistus incanus (Ci) herbal products inhibit human immunodeficiency virus (HIV) infections in vitro. Ci extract inhibited clinical HIV-1 and HIV-2 isolates, and, importantly, a virus isolate with multiple drug resistances, confirming broad anti-HIV activity. Antiviral activity was highly selective for virus particles, preventing primary attachment of the virus to the cell surface and viral envelope proteins from binding to heparin. Bioassay-guided fractionation indicated that Ci extract contains numerous antiviral compounds and therefore has favorably low propensity to induce virus resistance. Indeed, no resistant viruses emerged during 24 weeks of continuous propagation of the virus in the presence of Ci extracts. Finally, Ci extracts also inhibited infection by virus particles pseudotyped with Ebola and Marburg virus envelope proteins, indicating that antiviral activity of Ci extract extends to emerging viral pathogens. These results demonstrate that Ci extracts show potent and broad in vitro antiviral activity against viruses that cause life-threatening diseases in humans and are promising sources of agents that target virus particles.

Published
2016
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9. The root extract of the medicinal plant Pelargonium sidoides is a potent HIV-1 attachment inhibitor.

Author

Helfer M, Koppensteiner H, Schneider M, Rebensburg S, Forcisi S, Müller C, Schmitt-Kopplin P, Schindler M, and Brack-Werner R

Subjects
Anti-HIV Agents chemistry, Anti-HIV Agents isolation & purification, Drug Evaluation, Preclinical, HEK293 Cells, HIV Infections drug therapy, Humans, Plant Extracts chemistry, Plant Extracts isolation & purification, Plants, Medicinal chemistry, Polyphenols chemistry, Polyphenols isolation & purification, Polyphenols pharmacology, Anti-HIV Agents pharmacology, HIV-1 drug effects, Pelargonium chemistry, Plant Extracts pharmacology, Plant Roots chemistry, Virus Attachment drug effects
Abstract

Global HIV-1 treatment would benefit greatly from safe herbal medicines with scientifically validated novel anti-HIV-1 activities. The root extract from the medicinal plant Pelargonium sidoides (PS) is licensed in Germany as the herbal medicine EPs®7630, with numerous clinical trials supporting its safety in humans. Here we provide evidence from multiple cell culture experiments that PS extract displays potent anti-HIV-1 activity. We show that PS extract protects peripheral blood mononuclear cells and macrophages from infection with various X4 and R5 tropic HIV-1 strains, including clinical isolates. Functional studies revealed that the extract from PS has a novel mode-of-action. It interferes directly with viral infectivity and blocks the attachment of HIV-1 particles to target cells, protecting them from virus entry. Analysis of the chemical footprint of anti-HIV activity indicates that HIV-1 inhibition is mediated by multiple polyphenolic compounds with low cytotoxicity and can be separated from other extract components with higher cytotoxicity. Based on our data and its excellent safety profile, we propose that PS extract represents a lead candidate for the development of a scientifically validated herbal medicine for anti-HIV-1 therapy with a mode-of-action different from and complementary to current single-molecule drugs.

Published
2014
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10. [Sonography and biliary extracorporeal shockwave lithotripsy (ESWL)].

Author

Jakobeit C, Greiner L, Rebensburg S, Spelter M, Schumacher R, Frenzel F, and Pumplün B

Subjects
Cholelithiasis diagnostic imaging, Follow-Up Studies, Gallstones diagnostic imaging, Humans, Rupture, Spontaneous, Cholelithiasis therapy, Gallstones therapy, Lithotripsy, Ultrasonography
Abstract

Ultrasound is an indispensable tool for preliminary diagnosis ("filter function"), during treatment ("monitoring function") and in the follow-up examinations ("follow-up function") after shock-wave lithotripsy of gallstones. It permits rapid and reliable assessment of the therapeutic outcome and early identification of complications, which present-day experience has shown to be rare.

Published
1992
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11. [Ultrasound morphology of gallstones].

Author

Jakobeit CH, Rebensburg S, and Greiner L

Subjects
Artifacts, Bile Pigments analysis, Cholelithiasis chemistry, Cholelithiasis therapy, Cholesterol analysis, Crystallization, Humans, Lithotripsy, Prognosis, Ultrasonography, Cholelithiasis diagnostic imaging
Abstract

Using a subtile examination technique genuine information can be obtained from the interior of a gallstone--at least to a depth of 15 mm. This information should provide an indication of the homogeneous (crystalline) or inhomogeneous (non-cholesterol) structure of the stone. Further systematic use of differentiating gallstone ultrasonography could become a useful additional decision making criterion for selection of gallstones suitable for conservative treatment.

Published
1992

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