Your search keyword '"De Jong, Dorien"' showing total 5 results

1. Maraviroc is able to inhibit dual-R5 viruses in a dual/mixed HIV-1-infected patient.

Author

Symons, Jori, Van Lelyveld, Steven F. L., Hoepelman, Andy I. M., Van Ham, Petra M., De Jong, Dorien, Wensing, Annemarie M. J., and Nijhuis, Monique

Subjects

MARAVIROC (Drug), TREATMENT effectiveness, HIV, VIRAL replication, HIV infections, THERAPEUTICS, ANTIVIRAL agents, PREVENTION

Abstract

Objectives Maraviroc is the first licensed chemokine co-receptor 5 (CCR5) co-receptor antagonist in clinical practice. It is currently being used in patients harbouring exclusively CCR5-tropic virus. The objective of the study was to investigate the impact of maraviroc on viruses with different co-receptor preferences in a patient with a dual/mixed (D/M) infection. Methods We present a case report of an HIV-1 patient infected with a D/M virus population. Co-receptor tropism was determined by phenotypic and genotypic tests. Biological clones from pre- and post-maraviroc therapy were generated. Tropism of these infectious clones was investigated in U373-MAGI cells expressing CD4+ CCR5+ or CD4+ CXCR4+. Maraviroc susceptibility and viral replication were determined using donor peripheral blood mononuclear cells (PBMCs). Results In-depth clonal genotypic analysis revealed the presence of both R5-tropic variants and X4-tropic viruses before the start of maraviroc. During maraviroc therapy all R5-predicted viruses were suppressed. Phenotypic analyses revealed that all biological clones before maraviroc therapy could infect both CCR5- and CXCR4-bearing U373-MAGI cells, demonstrating dual tropism. The baseline biological clones preferentially infected the CCR5 cell line and were fully susceptible to maraviroc in PBMCs (dual-R5). In contrast, during maraviroc therapy the dual-R5-tropic viruses were replaced by more X4-tropic viruses (dual-X4), which could not be inhibited by maraviroc. Conclusions This case report demonstrates that dual-tropic viruses, capable of using both co-receptors in phenotypic assays, can be inhibited by maraviroc if they have a CCR5 co-receptor preference in vivo. [ABSTRACT FROM PUBLISHER]

Published

2011

2. Failure of Treatment with First-Line Lopinavir Boosted with Ritonavir Can Be Explained by Novel Resistance Pathways with Protease Mutation 76V.

Author

Nijhuis, Monique, Wensing, Annemarie M. J., Bierman, Wouter F. W., de Jong, Dorien, Kagan, Ron, Fun, Axel, Jaspers, Christian A. J. J., Schurink, Karin A. M., van Agtmael, Michael A., and Boucher, Charles A. B.

Subjects

PROTEOLYTIC enzymes, HIGHLY active antiretroviral therapy, HIV-positive persons, HIV, GENETICS, VIRAL replication

Abstract

Background. Virological failure of first-line antiretroviral therapy based on lopinavir boosted with ritonavir (lopinavir/r) has rarely been associated with resistance in protease. We identified a new genotypic resistance pathway in 3 patients who experienced failure of first-line lopinavir/r treatment. Methods. Viral protease and the C-term part of Gag were sequenced. The observed mutations were introduced in a reference strain to investigate impact on protease inhibitor susceptibility and replication capacity. Results. A detailed longitudinal analysis demonstrated the selection of the M46I+L76V protease mutations in all 3 patients. The L76V conferred a solitary 3.5-fold increase in one-half the maximal inhibitory concentration to lopinavir but severely hampered viral replication. Addition of M46I, which did not confer any lopinavir resistance on its own, had a dual effect. It partly compensated for the loss in replication capacity and increased the one-half maximal inhibitory concentration to above the lower clinical cutoff (11-fold). Analysis of a large clinical database (>180,000 human immunodeficiency virus [HIV] sequences) demonstrated a significant association (Spearman ρ, 0.93) between the increased presence of L76V in clinical samples (0.5% in 2000 to 3.4% in 2006) and lopinavir prescription over time. Conclusions. The HIV protease substitution L76V, in combination with M46I, confers clinically relevant levels of lopinavir resistance and represents a novel resistance pathway to first-line lopinavir/r therapy. [ABSTRACT FROM AUTHOR]

Published

2009

3. Persistence of HIV-1 Variants with Multiple Protease Inhibitor (PI)--Resistance Mutations in the Absence of PI Therapy Can Be Explained by Compensatory Fixation.

Author

Van Maarseveen, Noortje M., Wensing, Annemarie M. J., De Jong, Dorien, Taconis, Maaike, Borleffs, Jan C. C., Boucher, Charles A. B., and Nijhuis, Monique

Subjects

HIV infections, THERAPEUTICS, HIV, ANTIRETROVIRAL agents, RECOMBINANT viruses, ENZYME inhibitors, GENETIC mutation

Abstract

Objective. To investigate the mechanism explaining the persistence of human immunodeficiency virus (HIV) type 1 variants with multiple protease inhibitor (PI)-resistance mutations in the absence of PI therapy. Methods. Longitudinal genotypic analyses were performed on sequential samples obtained from 2 HIV-1-infected patients who had stopped PI therapy for 4 years. Replication capacity (RC) was determined using recombinant viruses. Subsequently, the effect that changing individual protease mutations back to wild type has on RC was analyzed. Results. We observed prolonged persistence (up to 4 years) of viruses with multiple protease mutations after PI therapy was stopped, despite the fact that the RC of the viruses was severely reduced. Forcing the virus to evolve toward wild type by changing individual protease mutations to wild type was unsuccessful, because all variants displayed a decreased RC in comparison with that of their predecessors. Conclusions. We propose compensatory fixation as a mechanism for the in vivo persistence of variants with multiple PI-resistance mutations in the absence of PI therapy. Viruses with multiple PI mutations have (partially) compensated for the initial loss in RC. Therefore, reversion of a single mutation causes a (further) reduction in RC and, as a consequence, the route to wild type is blocked. [ABSTRACT FROM AUTHOR]

Published

2007

4. Lamivudine-Resistant Human Immunodeficiency Virus Type 1 Variants (184V) Require Multiple Amino Acid Changes to Become Co-Resistant to Zidovudine In Vivo.

Author

Nijhuis, Monique, Schuurman, Rob, de Jong, Dorien, van Leeuwen, Remko, Lange, Joep, Danner, Sven, Keulen, Wilco, de Groot, Tom, and Boucher, Charles A. B.

Abstract

Exposure of human immunodeficiency virus to the nucleoside analogue lamivudine (3TC) rapidly selects for resistant variants with a valine at codon 184 (M184V) in the catalytic site of reverse transcriptase. In vitro, 184V demonstrated increased enzyme fidelity and suppressed zidovudine resistance. Clinical trials demonstrated that 3TC-zidovudine combination therapy results in a strong and sustained antiviral response. To investigate the role of 184V on in vivo virus evolution, the effect of zidovudine addition in 3TC-pretreated patients harboring 184V was studied. In vivo, no significant change in fidelity was observed with 184V, shown by generation of the classical pattern of zidovudine mutations. Of interest, in contrast to zidovudine monotherapy, in which just one substitution is sufficient for in vivo development of significant zidovudine resistance, multiple substi-tutions are required for the same level of zidovudine resistance in strains harboring 184V. This need for multiple substitutions may be one of the mechanisms explaining the sustained antiretroviral response of the 3TC-zidovudine combination. [ABSTRACT FROM PUBLISHER]

Published

1997

5. Rapid Changes in Human Immunodeficiency Virus Type 1 RNA Load and Appearance of Drug-Resistant Virus Populations in Persons Treated with Lamivudine (3TC).

Author

Schuurman, Rob, Nijhuis, Monique, van Leeuwen, Remko, Schipper, Pauline, de Jong, Dorien, Collis, Phil, Danner, Sven A., Mulder, John, Loveday, Clive, Christopherson, Cindy, Kwok, Shirley, Sninsky, John, and Boucher, Charles A. B.

Abstract

The effect of the appearance of drug-resistant human immunodeficiency virus type 1 (HIV-1) on viral RNA load was studied in patients treated with the reverse transcriptase inhibitor lamivudine. During the first 12 weeks of treatment, HIV-I RNA concentrations and amino acid changes in codon 184, causing high-level resistance to lamivudine, were determined in longitudinal serum samples from HIV-1 p24 antigen-positive and -negative patients. A marked decline in the amount of HIV-I RNA (∼95% below baseline) and HIV-I p24 antigen was observed within 2 weeks, followed by a rise that coincided with the appearance of lamivudine-resistant viruses in serum (isoleucine mutants initially, which were subsequently replaced by valine variants). After 12 weeks, a partial antiviral effect was observed despite the presence of a complete codon 184 mutant virus population in serum. This study shows that the rapid appearance of drug-resistant virus in serum is followed by an increase in viral RNA load. [ABSTRACT FROM PUBLISHER]

Published

1995