Your search keyword '"Sönnerborg, Anders"' showing total 17 results

1. Analysis of mutational history of multidrug‐resistant genotypes with a mutagenetic tree model.

Author

Pirkl, Martin, Büch, Joachim, Devaux, Carole, Böhm, Michael, Sönnerborg, Anders, Incardona, Francesca, Abecasis, Ana, Vandamme, Anne‐Mieke, Zazzi, Maurizio, Kaiser, Rolf, Lengauer, Thomas, and The EuResist Network Study Group

Subjects

SOMATIC mutation, HIV, MULTIDRUG resistance, REVERSE transcriptase, DRUG accessibility, MULTIDRUG-resistant tuberculosis

Abstract

Human immunodeficiency virus (HIV) can develop resistance to all antiretroviral drugs. Multidrug resistance, however, is a rare event in modern HIV treatment, but can be life‐threatening, particular in patients with very long therapy histories and in areas with limited access to novel drugs. To understand the evolution of multidrug resistance, we analyzed the EuResist database to uncover the accumulation of mutations over time. We hypothesize that the accumulation of resistance mutations is not acquired simultaneously and randomly across viral genotypes but rather tends to follow a predetermined order. The knowledge of this order might help to elucidate potential mechanisms of multidrug resistance. Our evolutionary model shows an almost monotonic increase of resistance with each acquired mutation, including less well‐known nucleoside reverse transcriptase (RT) inhibitor‐related mutations like K223Q, L228H, and Q242H. Mutations within the integrase (IN) (T97A, E138A/K G140S, Q148H, N155H) indicate high probability of multidrug resistance. Hence, these IN mutations also tend to be observed together with mutations in the protease (PR) and RT. We followed up with an analysis of the mutation‐specific error rates of our model given the data. We identified several mutations with unusual rates (PR: M41L, L33F, IN: G140S). This could imply the existence of previously unknown virus variants in the viral quasispecies. In conclusion, our bioinformatics model supports the analysis and understanding of multidrug resistance. [ABSTRACT FROM AUTHOR]

Published

2023

2. Evaluation of etravirine resistance in clinical samples by a simple phenotypic Test

Author

Agneskog, Eva, Nowak, Piotr, Källander, Clas F.R., and Sönnerborg, Anders

Published

2013

3. Increased replication capacity following evolution of PYxE insertion in Gag-p6 is associated with enhanced virulence in HIV-1 subtype C from East Africa

Author

Aralaguppe, Shambhu G., primary, Winner, Dane, additional, Singh, Kamalendra, additional, Sarafianos, Stefan G., additional, Quiñones-Mateu, Miguel E., additional, Sönnerborg, Anders, additional, and Neogi, Ujjwal, additional

Published

2016

4. Increased replication capacity following evolution of PYxE insertion in Gag-p6 is associated with enhanced virulence in HIV-1 subtype C from East Africa.

Author

Aralaguppe, Shambhu G., Winner, Dane, Singh, Kamalendra, Sarafianos, Stefan G., Quiñones‐Mateu, Miguel E., Sönnerborg, Anders, and Neogi, Ujjwal

Abstract

Background: A lower virulence of HIV-1 subtype C (HIV-1C) is suggested to be related to the global dominance of HIV-1C. In this observational study, combining in vivo (clinical monitoring) and in vitro (genotypic, biochemical, and phenotypic assays), we explored whether HIV-1C from East Africa (HIV-1CEA) is more pathogenic due to the evolution of a PYxE-insertion (CPYxEi) in the gag-p6 that also could affect the therapy response. Methods: HIV-1B (n = 112) and HIV-1CEA (n = 128)-infected individuals residing in Sweden were analyzed with regard to Gag-p6 genotype and clinically monitored. Based on the Gag-p6 characteristics, three HIV-1CEA and one HIV-1 B patient-derived p2-INT-recombinant virus (gag-p2/NCp7/p1/p6/pol-PR/RT/IN) were constructed to analyze viral growth kinetics (VGKs) and drug sensitivity assays. Reverse transcriptase (RT) from the same samples was cloned into the heterodimer expression plasmid (pRT6H-PROT) to analyze catalytic efficiency of RT. Results: A higher viral failure rate and lower pre-therapy CD4+ T-cell counts were observed in HIV-1CEA-infected patients compared to HIV-1B-infected patients. In Gag-p6, PTAP-duplication was more common in HIV-1C. HIV-1CEA-infected patients with signature CPYxEi, evidenced very low pre-therapy CD4+ T-cell counts and suboptimal gain in CD4+ T-cells following therapy, as compared to the non-CPYxEi-strains indicating higher virulence. VGKs showed a statistically significant higher replication capacity (RC) for the CPYxEi viruses than the other two non-CPYxEi strains. No statistically significant difference was observed in the catalytic efficiency among HIV-1C RTs. Conclusions: This is the first evidence of polymerase independent increased virulence and RC in HIV-1CEA following PYxE-insertion that is associated with suboptimal CD4+ T-cell gain following therapy initiation. J. Med. Virol. 89:106-111, 2017. © 2016 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2017

5. Selection of drug‐resistant HIV‐1 during the early phase of viral decay is uncommon in treatment‐naïve patients initiated on a three‐ or four‐drug antiretroviral regimen including lamivudine

Author

Bergroth, Tobias, primary, Ekici, Halime, additional, Gisslén, Magnus, additional, Loes, Sabine Kinloch‐de, additional, Goh, Li‐Ean, additional, Freedman, Andrew, additional, Lampe, Fiona, additional, Johnson, Margaret A., additional, and Sönnerborg, Anders, additional

Published

2008

6. Inter‐laboratory comparison of HCV‐RNA assay results: Implications for multi‐centre research

Author

Pembrey, Lucy, primary, Newell, Marie‐Louise, additional, Tovo, Pier‐Angelo, additional, van Drimmelen, Harry, additional, Quinti, Isabella, additional, Furlini, Giuliano, additional, Galli, Silvia, additional, Meliconi, Maria Grazia, additional, Burns, Sheila, additional, Hallam, Nick, additional, Sönnerborg, Anders, additional, Cilla, Gustavo, additional, Serrano, Esther, additional, Laccetti, Paolo, additional, Portella, Giuseppe, additional, Polywka, Susanne, additional, Icardi, Giancarlo, additional, Bruzzone, Bianca, additional, Balbo, Luciano, additional, and Alfarano, Alda, additional

Published

2002

7. Persistence of earlier HIV-1 drug resistance mutations at new treatment failure

Author

Svedhem, Veronica, primary, Lindkvist, Annica, additional, Lidman, Knut, additional, and Sönnerborg, Anders, additional

Published

2002

8. Variation in the hepatitis C virus NS5a region in relation to hypervariable region 1 heterogeneity during interferon treatment

Author

Odeberg, Jacob, primary, Yun, Zhibing, additional, Sönnerborg, Anders, additional, Weiland, Ola, additional, and Lundeberg, Joakim, additional

Published

1998

9. Discrepancy of hepatitis C virus genotypes as determined by phylogenetic analysis of partial NS5 and core sequences

Author

Yun, Zhibing, primary, Lara, Claudia, additional, Johansson, Bo, additional, Lorenzana de Rivera, Ivette, additional, and Sönnerborg, Anders, additional

Published

1996

10. Evaluation of a multiple peptide assay for typing of antibodies to the hepatitis C virus: Relation to genomic typing by the polymerase chain reaction

Author

Zhang, Zhu-Xu, primary, Yun, Zhi-Bing, additional, Chen, Margaret, additional, Sönnerborg, Anders, additional, and Sällberg, Matti, additional

Published

1995

11. Hepatitis C viral RNA titers in serum prior to, during, and after oral treatment with ribavirin for chronic hepatitis C

Author

Reichard, Olle, primary, Yun, Zhi-Bing, additional, Sönnerborg, Anders, additional, and Weiland, Ola, additional

Published

1993

12. Detection of hepatitis C virus (HCV) RNA by PCR related to HCV antibodies in serum and liver histology in swedish blood donors

Author

Yun, Zhi-Bing, primary, Lindh, Gudrun, additional, Weiland, Ola, additional, Johansson, Bo, additional, and Sönnerborg, Anders, additional

Published

1993

13. Selection of drug-resistant HIV-1 during the early phase of viral decay is uncommon in treatment-naïve patients initiated on a three- or four-drug antiretroviral regimen including lamivudine.

Author

Bergroth, Tobias, Ekici, Halime, Gisslén, Magnus, Loes, Sabine Kinloch-de, Goh, Li-Ean, Freedman, Andrew, Lampe, Fiona, Johnson, Margaret A., and Sönnerborg, Anders

Abstract

Therapy failure due to drug resistance development is a common phenomenon in HIV-infected patients. However, when the drug pressure leads to the earliest selection of drug-resistant HIV-1 populations is still unclear. In this study, the extent to which selection of the HIV-1 reverse transcriptase M184I/V mutations occur during the initial phase of viral decay in treatment-naïve HIV-1 infected patients receiving antiretroviral therapy (ART) was examined. Plasma virus from three cohorts of treatment-naïve patients initiating quadruple (n = 43), triple (n = 14) or dual (n = 15) lamivudine-containing ART were analyzed for M184I/V during the first 6 months of therapy using direct sequencing and a sensitive selective real-time PCR method. Among quadruple ART patients, who all were treated at primary HIV-1 infection, only one patient developed M184V after 6 weeks of therapy, having had wild-type virus at baseline. No mutations were found in chronically infected patients on triple ART. In patients on dual therapy, M184I/V mutants were found frequently. Selection of M184I/V mutants was found to be rare during the initial phase of viral decay after initiation of ART in adherent patients given a three or four-drug combination, in contrast to those receiving a less potent regimen. The results suggest that triple and quadruple lamivudine + PI or PI/r containing ART given to treatment-naïve adherent patients is potent enough to prevent development of resistance during the first months of therapy. J. Med. Virol. 81:1-8, 2009. © 2008 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

14. Detection of human immunodeficiency virus-1 by polymerase chain reaction and virus cultivation

Author

Sönnerborg, Anders, primary, Abens, Janis, additional, Johansson, Bo, additional, and Strannegård, Örjan, additional

Published

1990

15. Inter-laboratory comparison of HCV-RNA assay results: Implications for multi-centre research.

Author

Pembrey, Lucy, Newell, Marie-Louise, Tovo, Pier-Angelo, van Drimmelen, Harry, Quinti, Isabella, Furlini, Giuliano, Galli, Silvia, Meliconi, Maria Grazia, Burns, Sheila, Hallam, Nick, Sönnerborg, Anders, Cilla, Gustavo, Serrano, Esther, Laccetti, Paolo, Portella, Giuseppe, Polywka, Susanne, Icardi, Giancarlo, Bruzzone, Bianca, Balbo, Luciano, and Alfarano, Alda

Published

2003

16. IgG subclass reactivity against human immunodeficiency virus (HIV) and cytomegalovirus in cerebrospinal fluid and serum from HIV-infected patients.

Author

Mathiesen, Tiit, Sönnerborg, Anders, Sydow, Madeleine Von, Gaines, Hans, and Wahren, Britta

Published

1988

17. Isolation of human immunodeficiency virus (HIV) from plasma during primary HIV infection.

Author

Albert, Jan, Gaines, Hans, Sönnerborg, Anders, Nyström, Gunnel, Pehrson, Pehr Olov, Chiodi, Francesca, von Sydow, Madeleine, Moberg, Lars, Lidman, Knut, Christensson, Bertil, Åsjö, Birgitta, and Fenyö, Eva Maria

Published

1987