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1. Correction: Effects of spermidine supplementation on cognition and biomarkers in older adults with subjective cognitive decline (SmartAge)—study protocol for a randomized controlled trial

Author

Wirth, Miranka, Schwarz, Claudia, Benson, Gloria, Horn, Nora, Buchert, Ralph, Lange, Catharina, Köbe, Theresa, Hetzer, Stefan, Maglione, Marta, Michael, Eva, Märschenz, Stefanie, Mai, Knut, Kopp, Ute, Schmitz, Dietmar, Grittner, Ulrike, Sigrist, Stephan J., Stekovic, Slaven, Madeo, Frank, and Flöel, Agnes

Published
2022
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2. Effects of spermidine supplementation on cognition and biomarkers in older adults with subjective cognitive decline (SmartAge)—study protocol for a randomized controlled trial

Author

Wirth, Miranka, Schwarz, Claudia, Benson, Gloria, Horn, Nora, Buchert, Ralph, Lange, Catharina, Köbe, Theresa, Hetzer, Stefan, Maglione, Marta, Michael, Eva, Märschenz, Stefanie, Mai, Knut, Kopp, Ute, Schmitz, Dietmar, Grittner, Ulrike, Sigrist, Stephan J., Stekovic, Slaven, Madeo, Frank, and Flöel, Agnes

Published
2019
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3. Hepatitis D Virus (HDV)

Author

Meisel, Helga, Märschenz, Stefanie, Krüger, Detlev H., Darai, Gholamreza, editor, Handermann, Michaela, editor, Sonntag, Hans-Günther, editor, Tidona, Christian A., editor, and Zöller, Lothar, editor

Published
2009
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4. Hepatitis C Virus (HCV)

Author

Meisel, Helga, Märschenz, Stefanie, Krüger, Detlev H., Darai, Gholamreza, editor, Handermann, Michaela, editor, Sonntag, Hans-Günther, editor, Tidona, Christian A., editor, and Zöller, Lothar, editor

Published
2009
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5. Hepatitis B Virus (HBV)

Author

Meisel, Helga, Märschenz, Stefanie, Krüger, Detlev H., Darai, Gholamreza, editor, Handermann, Michaela, editor, Sonntag, Hans-Günther, editor, Tidona, Christian A., editor, and Zöller, Lothar, editor

Published
2009
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6. Rationale and design of the prevention of paclitaxel-related neurological side effects with lithium trial – Protocol of a multicenter, randomized, double-blind, placebo- controlled proof-of-concept phase-2 clinical trial

Author

Huehnchen, Petra, primary, Bangemann, Nikola, additional, Lischewski, Sandra, additional, Märschenz, Stefanie, additional, Paul, Friedemann, additional, Schmitz-Hübsch, Tanja, additional, Blohmer, Jens-Uwe, additional, Eberhardt, Cornelia, additional, Rauch, Geraldine, additional, Flöel, Agnes, additional, Adam, Sophie, additional, Schwenkenbecher, Philipp, additional, Meinhold-Heerlein, Ivo, additional, Hoffmann, Oliver, additional, Ziemssen, Tjalf, additional, Endres, Matthias, additional, and Boehmerle, Wolfgang, additional

Published
2022
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7. Effects of Spermidine Supplementation on Cognition and Biomarkers in Older Adults With Subjective Cognitive Decline

Author

Schwarz, Claudia, primary, Benson, Gloria S., additional, Horn, Nora, additional, Wurdack, Katharina, additional, Grittner, Ulrike, additional, Schilling, Ralph, additional, Märschenz, Stefanie, additional, Köbe, Theresa, additional, Hofer, Sebastian J., additional, Magnes, Christoph, additional, Stekovic, Slaven, additional, Eisenberg, Tobias, additional, Sigrist, Stephan J., additional, Schmitz, Dietmar, additional, Wirth, Miranka, additional, Madeo, Frank, additional, and Flöel, Agnes, additional

Published
2022
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10. Simvastatin add-on to escitalopram in patients with comorbid obesity and major depression (SIMCODE): study protocol of a multicentre, randomised, double-blind, placebo-controlled trial

Author

Otte, Christian, Chae, Woo Ri, Nowacki, Jan, Kaczmarczyk, Michael, Piber, Dominique, Roepke, Stefan, Märschenz, Stefanie, Lischewski, Sandra, Schmidt, Sein, Ettrich, Barbara, Grabe, Hans Joergen, Hegerl, Ulrich, Hinkelmann, Kim, Hofmann, Tobias, Janowitz, Deborah, Junghanns, Klaus, Kahl, Kai G, Klein, Jan Philipp, Krueger, Tillmann H C, Leicht, Gregor, Prvulovic, David, Reif, Andreas, Schoettle, Daniel, Strauss, Maria, Westermair, Anna, Friede, Tim, Gold, Stefan M, University of Zurich, and Otte, Christian

Subjects
Depressive Disorder, Major, Simvastatin, clinical trials, Depression, 610 Medicine & health, 2700 General Medicine, General Medicine, Citalopram, Berlin, Treatment Outcome, Double-Blind Method, depression & mood disorders, mental disorders, 10222 Institute of Biomedical Ethics and History of Medicine, Humans, Multicenter Studies as Topic, Obesity, mental health, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, Randomized Controlled Trials as Topic
Abstract

Introduction Major depressive disorder (MDD) and obesity are both common disorders associated with significant burden of disease worldwide. Importantly, MDD and obesity often co-occur, with each disorder increasing the risk for developing the other by about 50%–60%. Statins are among the most prescribed medications with well-established safety and efficacy. Statins are recommended in primary prevention of cardiovascular disease, which has been linked to both MDD and obesity. Moreover, statins are promising candidates to treat MDD because a meta-analysis of pilot randomised controlled trials has found antidepressive effects of statins as adjunct therapy to antidepressants. However, no study so far has tested the antidepressive potential of statins in patients with MDD and comorbid obesity. Importantly, this is a difficult-to-treat population that often exhibits a chronic course of MDD and is more likely to be treatment resistant. Thus, in this confirmatory randomised controlled trial, we will determine whether add-on simvastatin to standard antidepressant medication with escitalopram is more efficacious than add-on placebo over 12 weeks in 160 patients with MDD and comorbid obesity. Methods and analysis This is a protocol for a randomised, placebo-controlled, double-blind multicentre trial with parallel-group design (phase II). One hundred and sixty patients with MDD and comorbid obesity will be randomised 1:1 to simvastatin or placebo as add-on to standard antidepressant medication with escitalopram. The primary outcome is change in the Montgomery-Åsberg Depression Rating Scale (MADRS) score from baseline to week 12. Secondary outcomes include MADRS response (defined as 50% MADRS score reduction from baseline), MADRS remission (defined as MADRS score

Published
2020

13. Simvastatin add-on to escitalopram in patients with comorbid obesity and major depression (SIMCODE): study protocol of a multicentre, randomised, double-blind, placebo-controlled trial

Author

Otte, Christian, primary, Chae, Woo Ri, additional, Nowacki, Jan, additional, Kaczmarczyk, Michael, additional, Piber, Dominique, additional, Roepke, Stefan, additional, Märschenz, Stefanie, additional, Lischewski, Sandra, additional, Schmidt, Sein, additional, Ettrich, Barbara, additional, Grabe, Hans Joergen, additional, Hegerl, Ulrich, additional, Hinkelmann, Kim, additional, Hofmann, Tobias, additional, Janowitz, Deborah, additional, Junghanns, Klaus, additional, Kahl, Kai G., additional, Klein, Jan Philipp, additional, Krueger, Tillmann H. C., additional, Leicht, Gregor, additional, Prvulovic, David, additional, Reif, Andreas, additional, Schoettle, Daniel, additional, Strauss, Maria, additional, Westermair, Anna, additional, Friede, Tim, additional, and Gold, Stefan M, additional

Published
2020
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14. Simvastatin add-on to escitalopram in patients with comorbid obesity and major depression (SIMCODE): study protocol of a multicentre, randomised, double-blind, placebo-controlled trial

Author

Otte, Christian; https://orcid.org/0000-0002-4051-997X, Chae, Woo Ri; https://orcid.org/0000-0002-6326-8333, Nowacki, Jan, Kaczmarczyk, Michael, Piber, Dominique, Roepke, Stefan, Märschenz, Stefanie; https://orcid.org/0000-0003-3303-5819, Lischewski, Sandra, Schmidt, Sein, Ettrich, Barbara, Grabe, Hans Joergen, Hegerl, Ulrich, Hinkelmann, Kim, Hofmann, Tobias, Janowitz, Deborah, Junghanns, Klaus, Kahl, Kai G, Klein, Jan Philipp; https://orcid.org/0000-0001-9882-2261, Krueger, Tillmann H C, Leicht, Gregor, Prvulovic, David, Reif, Andreas, Schoettle, Daniel, Strauss, Maria, Westermair, Anna; https://orcid.org/0000-0002-3673-4589, Friede, Tim; https://orcid.org/0000-0001-5347-7441, Gold, Stefan M; https://orcid.org/0000-0001-5188-4799, Otte, Christian; https://orcid.org/0000-0002-4051-997X, Chae, Woo Ri; https://orcid.org/0000-0002-6326-8333, Nowacki, Jan, Kaczmarczyk, Michael, Piber, Dominique, Roepke, Stefan, Märschenz, Stefanie; https://orcid.org/0000-0003-3303-5819, Lischewski, Sandra, Schmidt, Sein, Ettrich, Barbara, Grabe, Hans Joergen, Hegerl, Ulrich, Hinkelmann, Kim, Hofmann, Tobias, Janowitz, Deborah, Junghanns, Klaus, Kahl, Kai G, Klein, Jan Philipp; https://orcid.org/0000-0001-9882-2261, Krueger, Tillmann H C, Leicht, Gregor, Prvulovic, David, Reif, Andreas, Schoettle, Daniel, Strauss, Maria, Westermair, Anna; https://orcid.org/0000-0002-3673-4589, Friede, Tim; https://orcid.org/0000-0001-5347-7441, and Gold, Stefan M; https://orcid.org/0000-0001-5188-4799

Abstract

Introduction Major depressive disorder (MDD) and obesity are both common disorders associated with significant burden of disease worldwide. Importantly, MDD and obesity often co-occur, with each disorder increasing the risk for developing the other by about 50%–60%. Statins are among the most prescribed medications with well-established safety and efficacy. Statins are recommended in primary prevention of cardiovascular disease, which has been linked to both MDD and obesity. Moreover, statins are promising candidates to treat MDD because a meta-analysis of pilot randomised controlled trials has found antidepressive effects of statins as adjunct therapy to antidepressants. However, no study so far has tested the antidepressive potential of statins in patients with MDD and comorbid obesity. Importantly, this is a difficult-to-treat population that often exhibits a chronic course of MDD and is more likely to be treatment resistant. Thus, in this confirmatory randomised controlled trial, we will determine whether add-on simvastatin to standard antidepressant medication with escitalopram is more efficacious than add-on placebo over 12 weeks in 160 patients with MDD and comorbid obesity. Methods and analysis This is a protocol for a randomised, placebo-controlled, double-blind multicentre trial with parallel-group design (phase II). One hundred and sixty patients with MDD and comorbid obesity will be randomised 1:1 to simvastatin or placebo as add-on to standard antidepressant medication with escitalopram. The primary outcome is change in the Montgomery-Åsberg Depression Rating Scale (MADRS) score from baseline to week 12. Secondary outcomes include MADRS response (defined as 50% MADRS score reduction from baseline), MADRS remission (defined as MADRS score <10), mean change in patients’ self-reported Beck Depression Inventory (BDI-II) and mean change in high-density lipoprotein, low-density lipoprotein and total cholesterol from baseline to week 12. Ethics and disseminati

Published
2020

15. Bortezomib in antibody-mediated autoimmune diseases (TAVAB): study protocol for a unicentric, non-randomised, non-placebo controlled trial

Author

Kohler, Siegfried, Märschenz, Stefanie, Grittner, Ulrike, Alexander, Tobias, Hiepe, Falk, and Meisel, Andreas

Subjects
neurology, neuromuscular disease, Proof of Concept Study, Arthritis, Rheumatoid, Bortezomib, immunology, Rheumatology, Myasthenia Gravis, Protocol, Humans, Lupus Erythematosus, Systemic, Proteasome Inhibitors, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, Autoantibodies
Abstract

Introduction: The clinical characteristics of autoantibodymediated autoimmune diseases are diverse. Yet, medical treatment and the associated complications are similar, that is, the occurrence of long-term side effects and the problem that a significant proportion of patients are non-responders. Therefore, new therapeutic options are needed. Bortezomib, a proteasome inhibitor, is effective in the treatment of multiple myeloma and data from experimental models and case reports suggest an effect in the treatment of autoantibody-mediated autoimmunity. In our study, we will determine the effect of bortezomib treatment on a shared surrogate parameter for clinical efficacy, namely change in autoantibody levels, which we chose as primary parameter. Methods and analysis: We designed a phase IIa trial with altogether n=18 treatment-refractory patients suffering from myasthenia gravis, systemic lupus erythematosus and rheumatoid arthritis that will be treated with bortezomib add-on to pre-existing therapy. Primary endpoint is the change in autoantibody levels 6 months after therapy. Secondary endpoints include concomitant medication, disease-specific clinical scores and measures of quality of life and activities of daily living. Ethics and dissemination: Safety parameters include neurophysiological and clinical signs of peripheral neuropathy as well as potential central nervous system side effects determined by olfactory and neuropsychological testing. The study has been approved by the local ethical committee and first participants have already been enrolled. This proof of concept study will contribute to improve our understanding of plasma cellspecific treatment approaches by assessing its safety and efficacy in reducing serum levels of antibodies known to mediate autoimmune disorders. We plan to publish the final results of our study in a peer reviewed journal and to present our findings at international conferences. Trial registration number: NCT02102594.

Published
2019

18. Bortezomib in antibody-mediated autoimmune diseases (TAVAB): study protocol for a unicentric, nonrandomised, non-placebo controlled trial.

Author

Kohler, Siegfried, Märschenz, Stefanie, Grittner, Ulrike, Alexander, Tobias, Hiepe, Falk, and Meisel, Andreas

Abstract

Introduction The clinical characteristics of autoantibodymediated autoimmune diseases are diverse. Yet, medical treatment and the associated complications are similar, that is, the occurrence of long-term side effects and the problem that a significant proportion of patients are non-responders. Therefore, new therapeutic options are needed. Bortezomib, a proteasome inhibitor, is effective in the treatment of multiple myeloma and data from experimental models and case reports suggest an effect in the treatment of autoantibody-mediated autoimmunity. In our study, we will determine the effect of bortezomib treatment on a shared surrogate parameter for clinical efficacy, namely change in autoantibody levels, which we chose as primary parameter. Methods and analysis We designed a phase IIa trial with altogether n=18 treatment-refractory patients suffering from myasthenia gravis, systemic lupus erythematosus and rheumatoid arthritis that will be treated with bortezomib add-on to pre-existing therapy. Primary endpoint is the change in autoantibody levels 6 months after therapy. Secondary endpoints include concomitant medication, disease-specific clinical scores and measures of quality of life and activities of daily living. Ethics and dissemination Safety parameters include neurophysiological and clinical signs of peripheral neuropathy as well as potential central nervous system side effects determined by olfactory and neuropsychological testing. The study has been approved by the local ethical committee and first participants have already been enrolled. This proof of concept study will contribute to improve our understanding of plasma cellspecific treatment approaches by assessing its safety and efficacy in reducing serum levels of antibodies known to mediate autoimmune disorders. We plan to publish the final results of our study in a peer reviewed journal and to present our findings at international conferences. [ABSTRACT FROM AUTHOR]

Published
2019
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19. Funktionelle Analyse von komplexen Hepatitis-B-Virus-Varianten, assoziiert mit Leberzirrhose bei Immunsupprimierten

Author

Märschenz, Stefanie, Krüger, Detlev H., Schönrich, Günther, and Jilg, Wolfgang

Subjects
variants, Leberzirrhose, phenotype, Varianten, liver cirrhosis, pathogenesis, funktionelle Analyse, Nierentransplantatempfänger, Transfektion, 32 Biologie, Phänotyp, Hepatitis B Virus (HBV), functional analysis, renal transplant recipients, Pathogenese, transfection, ddc:570, hepatoma cell line, XD 7304, immunsupprimiert, 570 Biowissenschaften, Biologie, Hepatomazelllinie, immuno-suppressed
Abstract

Obwohl der Wildtyp des Hepatitis-B-Virus (HBV) nicht zytopathogen und die Pathogenese der Hepatitis B generell immunvermittelt ist, können in immunsupprimierten Nierentransplantatempfängern mit chronischer Hepatitis B schwere Leberschäden bis hin zu Leberzirrhose und Leberversagen entstehen. Die Entwicklung von Leberzirrhose in den Nierentransplantierten ist assoziiert mit der Akkumulation und Persistenz von komplexen HBV-Varianten mit Mutationen im Core-Promotor / X-Gen, Deletionen im Core (C)-Gen und teilweise zusätzlichen Deletionen im präS-Bereich. Dies lässt eine Rolle der Varianten in der speziellen Pathogenese bei Immunsupprimierten vermuten. In der vorliegenden Arbeit wurden funktionelle Analysen der komplexen Varianten im Vergleich zu Referenz-Wildtypgenomen und Wildtyp-ähnlichen Genomen der Patienten aus der frühen Infektionsphase durchgeführt, um Hinweise auf den potentiellen Beitrag der Varianten zur Pathogenese zu erlangen. Die Analysen erfolgten durch transiente Transfektion der humanen Hepatomazelllinie HuH7 mit repräsentativen HBV-Gesamtgenomen, die aus 2 Patienten während des Krankheitsverlaufs von einer asymptomatischen Infektion hin zur Leberzirrhose isoliert und kloniert worden waren. Trotz einiger Unterschiede im Detail wiesen die komplexen Varianten einen gemeinsamen, drastisch vom Wildtyp abweichenden Phänotyp auf. Dieser war gekennzeichnet durch eine veränderte Transkription mit reduzierten präC- und Oberflächen-mRNAs und verstärkter Expression der prägenomischen RNA, eine starke Reduktion des häufigsten Spleißprodukts der prägenomischen RNA, SP1, eine extrem reduzierte oder fehlende Expression und/oder Sekretion aller Oberflächenproteine und des HBeAg, ein verändertes intrazelluläres Verteilungsmuster des schwach exprimierten Core-Proteins und teilweise der Oberflächenproteine sowie eine erhöhte Replikation und Anreicherung gegenüber Wildtyp-HBV aufgrund einer verstärkten reversen Transkription der prägenomischen RNA. Dieser Phänotyp basierte zum Teil auf den Mutationen in Core-Promotor und C-Gen, wurde jedoch deutlich durch zusätzliche Mutationen in den übrigen Genomabschnitten beeinflusst. Die vielfältigen Veränderungen der Varianten unterstützen ihren vermuteten Beitrag zur Pathogenese. Although wild-type hepatitis B virus is not cytopathogenic and the pathogenesis of hepatitis B is generally immune mediated, also immuno-suppressed patients, such as renal transplant recipients, with chronic hepatitis B may develop liver cirrhosis and end-stage liver disease. In renal transplant recipients, the development of liver cirrhosis is associated with the accumulation and persistence of complex HBV variants with mutations in core promoter / X gene, deletions in core (C) gene and sometimes additional deletions in the preS region. This suggests a role of these variants in the special pathogenesis in immuno-suppressed patients. In the present work, the complex variants were functionally analyzed in comparison to reference wild-type genomes and wild-type-like HBV genomes from the early asymptomatic phase of infection. For the analyses, representative cloned full-length HBV genomes isolated from 2 patients before and during liver cirrhosis were transiently transfected into the human hepatoma cell line HuH7. In spite of some variations, the complex variants showed a common phenotype, which was drastically altered compared to wild-type. It was characterized by reduced preC and surface mRNAs and increased expression of pregenomic RNA, by a strong reduction of the major spliced pregenomic RNA, SP1, by a partial or complete defect in expression and/or secretion of surface proteins and HBeAg, by an aberrant intracellular localization of the weakly expressed core protein and in some cases of the surface proteins, and by an enhanced replication and enrichment over wild-type HBV due to an enhanced reverse transcription of variant pregenomic RNA. The phenotypic alterations were often based on the mutations in core promoter and C gene but were considerably influenced by the additional mutations in other genomic regions. The multiple functional changes of the variants support their assumed contribution to pathogenesis.

Published
2006

20. Funktionelle Analyse von komplexen Hepatitis-B-Virus-Varianten, assoziiert mit Leberzirrhose bei Immunsupprimierten

Author

Krüger, Detlev H., Schönrich, Günther, Jilg, Wolfgang, Märschenz, Stefanie, Krüger, Detlev H., Schönrich, Günther, Jilg, Wolfgang, and Märschenz, Stefanie

Abstract

Obwohl der Wildtyp des Hepatitis-B-Virus (HBV) nicht zytopathogen und die Pathogenese der Hepatitis B generell immunvermittelt ist, können in immunsupprimierten Nierentransplantatempfängern mit chronischer Hepatitis B schwere Leberschäden bis hin zu Leberzirrhose und Leberversagen entstehen. Die Entwicklung von Leberzirrhose in den Nierentransplantierten ist assoziiert mit der Akkumulation und Persistenz von komplexen HBV-Varianten mit Mutationen im Core-Promotor / X-Gen, Deletionen im Core (C)-Gen und teilweise zusätzlichen Deletionen im präS-Bereich. Dies lässt eine Rolle der Varianten in der speziellen Pathogenese bei Immunsupprimierten vermuten. In der vorliegenden Arbeit wurden funktionelle Analysen der komplexen Varianten im Vergleich zu Referenz-Wildtypgenomen und Wildtyp-ähnlichen Genomen der Patienten aus der frühen Infektionsphase durchgeführt, um Hinweise auf den potentiellen Beitrag der Varianten zur Pathogenese zu erlangen. Die Analysen erfolgten durch transiente Transfektion der humanen Hepatomazelllinie HuH7 mit repräsentativen HBV-Gesamtgenomen, die aus 2 Patienten während des Krankheitsverlaufs von einer asymptomatischen Infektion hin zur Leberzirrhose isoliert und kloniert worden waren. Trotz einiger Unterschiede im Detail wiesen die komplexen Varianten einen gemeinsamen, drastisch vom Wildtyp abweichenden Phänotyp auf. Dieser war gekennzeichnet durch eine veränderte Transkription mit reduzierten präC- und Oberflächen-mRNAs und verstärkter Expression der prägenomischen RNA, eine starke Reduktion des häufigsten Spleißprodukts der prägenomischen RNA, SP1, eine extrem reduzierte oder fehlende Expression und/oder Sekretion aller Oberflächenproteine und des HBeAg, ein verändertes intrazelluläres Verteilungsmuster des schwach exprimierten Core-Proteins und teilweise der Oberflächenproteine sowie eine erhöhte Replikation und Anreicherung gegenüber Wildtyp-HBV aufgrund einer verstärkten reversen Transkription der prägenomischen RNA. Dieser Phänotyp basiert, Although wild-type hepatitis B virus is not cytopathogenic and the pathogenesis of hepatitis B is generally immune mediated, also immuno-suppressed patients, such as renal transplant recipients, with chronic hepatitis B may develop liver cirrhosis and end-stage liver disease. In renal transplant recipients, the development of liver cirrhosis is associated with the accumulation and persistence of complex HBV variants with mutations in core promoter / X gene, deletions in core (C) gene and sometimes additional deletions in the preS region. This suggests a role of these variants in the special pathogenesis in immuno-suppressed patients. In the present work, the complex variants were functionally analyzed in comparison to reference wild-type genomes and wild-type-like HBV genomes from the early asymptomatic phase of infection. For the analyses, representative cloned full-length HBV genomes isolated from 2 patients before and during liver cirrhosis were transiently transfected into the human hepatoma cell line HuH7. In spite of some variations, the complex variants showed a common phenotype, which was drastically altered compared to wild-type. It was characterized by reduced preC and surface mRNAs and increased expression of pregenomic RNA, by a strong reduction of the major spliced pregenomic RNA, SP1, by a partial or complete defect in expression and/or secretion of surface proteins and HBeAg, by an aberrant intracellular localization of the weakly expressed core protein and in some cases of the surface proteins, and by an enhanced replication and enrichment over wild-type HBV due to an enhanced reverse transcription of variant pregenomic RNA. The phenotypic alterations were often based on the mutations in core promoter and C gene but were considerably influenced by the additional mutations in other genomic regions. The multiple functional changes of the variants support their assumed contribution to pathogenesis.

Published
2006

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