Virologic, immunologic, and clinical follow-up of a couple infected by the human immunodeficiency virus type one, group O

Nkengasong, John N.; Fransen, Katrien; Willems, Betty; Karita, Etienne; Vingerhoets, J.; Kestens, Luc; Colebunders, Robert; Piot, Peter; Groen, G van der

doi:10.1002/(sici)1096-9071(199703)51:3<202::aid-jmv10>3.0.co;2-m

Cited by 17 publications

(7 citation statements)

References 40 publications

(38 reference statements)

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“…Infection by CCR5-using HIV-1 and the late appearance of CXCR4-using HIV in disease have also been studied in patients infected with HIV-1 group M. However, the prevalence and evolution of HIV-1 using specific coreceptors in group O infections are still poorly understood as only very few group O-infected subjects have been followed during disease. 48 This of course also has relevance to the use of MVC in group O-infected individuals. To further our knowledge on coreceptor usage among group O isolates, U87.CD4.CCR5 or CXCR4 cells were exposed to each of the 18 HIV-1 group O primary isolates and 1 group M/O (Tables 1 and 2).…”

Section: Susceptibility Of Hiv-1 Group O To Mvc Inhibitionmentioning

confidence: 98%

HIV-1 Group O Genotypes and Phenotypes: Relationship to Fitness and Susceptibility to Antiretroviral Drugs

Tebit

Patel

Ratcliff

et al. 2016

AIDS Research and Human Retroviruses

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Despite only 30,000 group O HIV-1 infections, a similar genetic diversity is observed among the O subgroups H (head) and T (tail) (previously described as subtypes A, B) as in the 9 group M subtypes (A-K). Group O isolates bearing a cysteine at reverse transcriptase (RT) position 181, predominantly the H strains are intrinsically resistant to non-nucleoside reverse transcriptase inhibitors (NNRTIs). However, their susceptibility to newer antiretroviral drugs such as etravirine, maraviroc, raltegravir (RAL), and elvitegravir (EVG) remains relatively unknown. We tested a large collection of HIV-1 group O strains for their susceptibility to four classes of antiretroviral drugs namely nucleoside RT, non-nucleoside RT, integrase, and entry inhibitors knowing in advance the intrinsic resistance to NNRTIs. Drug target regions were sequenced to determine various polymorphisms and were phylogenetically analyzed. Replication kinetics and fitness assays were performed in U87-CD4(+)CCR5 and CXCR4 cells and peripheral blood mononuclear cells. With all antiretroviral drugs, group O HIV-1 showed higher variability in IC50 values than group M HIV-1. The mean IC50 values for entry and nucleoside reverse transcriptase inhibitor (NRTI) were similar for group O and M HIV-1 isolates. Despite similar susceptibility to maraviroc, the various phenotypic algorithms failed to predict CXCR4 usage based on the V3 Env sequences of group O HIV-1 isolates. Decreased sensitivity of group O HIV-1 to integrase or NNRTIs had no relation to replicative fitness. Group O HIV-1 isolates were 10-fold less sensitive to EVG inhibition than group M HIV-1. These findings suggest that in regions where HIV-1 group O is endemic, first line treatment regimens combining two NRTIs with RAL may provide more sustained virologic responses than the standard regimens involving an NNRTI or protease inhibitors.

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Section: Susceptibility Of Hiv-1 Group O To Mvc Inhibitionmentioning

confidence: 98%

HIV-1 Group O Genotypes and Phenotypes: Relationship to Fitness and Susceptibility to Antiretroviral Drugs

Tebit

Patel

Ratcliff

et al. 2016

AIDS Research and Human Retroviruses

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“…Before therapy, after 7 years of follow-up, the viral RNA levels in the asymptomatic individual A were 2.5-2.8 log 10 copies of RNA per milliliter, and CD4 1 T cell counts had decreased from 500 to 150 cells/ml. 5 Individual B had lymphoadenopathy, baseline viral RNA levels between 3.1 and 3.6 log 10 copies/ml, and a concomitant decline in CD4 1 T cell count from 500 to 20-50/ml. The clinical stage, the assessed viral RNA levels, and CD4 1 T cell counts of both individuals were within the range of clinical parameters found in group M-infected persons.…”

Section: Discussionmentioning

confidence: 99%

“…Individual B developed lymphadenopathy, three episodes of furunculosis, and intertrigo, with CD4 1 T cell counts declining from 500 to 20-50 cells/ml. 5 Serum samples were taken from both individuals just before start of therapy (day 1) and at intervals during treatment. These samples were stored at 270°C, along with serum samples from the period between seroconversion and start of therapy, until used for analysis of HIV-1 RNA levels.…”

Section: Two Hiv-1 Group O-infected Individualsmentioning

confidence: 99%

“…4 Although a relatively small number of group O-infected individuals has been monitored, the natural history of the group O viruses does not appear to differ substantially from that of group M viruses. 5 We have monitored the course of ANT70 infection in the index case (individual A) and her partner (individual B) since 1990. Both individuals have received antiviral therapy since 1995.…”

Section: Introductionmentioning

confidence: 99%

“…To date, the effect of antiviral therapy in such individuals has been examined primarily by the assessment of CD4 1 T cell counts and the approximation of HIV-1 group O RNA levels using a semiquantitative RNA assay that is able to detect group O virus infection. 5 The CD4 1 T cell count is an important marker, 11,12 but because of wide fluctuation it is insufficient to evaluate the effect of antiviral therapy. 13,14 Therefore, we developed a quantitative group O-specific viral RNA assay based on nucleic acid sequence-based amplification (NASBA) technology, with primers and probes validated for the ANT70 sequence.…”

Section: Introductionmentioning

confidence: 99%

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Natural Residues versus Antiretroviral Drug-Selected Mutations in HIV Type 1 Group O Reverse Transcriptase and Protease Related to Virological Drug Failurein Vivo

Baar

Janssens

Ronde

et al. 2000

AIDS Research and Human Retroviruses

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HIV-1 group O viruses were first recognized as a distinct subgroup of HIV-1 with the isolation and characterization in 1990 of a virus (ANT70) from a woman (individual A) and her spouse (individual B), both from Cameroon (De Leys R, et al.: J Virol 1990;64:1207-1216). During the 5-6 years before treatment, individual A remained asymptomatic, with viral RNA levels between 2.5 and 2.8 log10 copies/ml, as measured by a newly developed group O-specific quantitative NASBA-based RNA assay. Individual B developed mild clinical symptoms, with 3.1 to 3.6 log10 copies of viral RNA per milliliter. HIV-1 sequences obtained from both individuals showed pretreatment residues in protease that confer resistance to protease inhibitors in group M viruses (10I, 36I, and 71V). Individual A showed an initial response to AZT, but shortly after addition of ddC and saquinavir, the RNA levels returned to baseline, while subsequent treatment with d4T, 3TC, and indinavir reduced the RNA level to less than 50 copies/ml for the time of follow-up. Individual B showed no response to AZT or ddC monotherapy, and a change to d4T, 3TC, and indinavir had, in contrast to individual A, only a temporary effect. While a multitude of mutations in HIV-1 group O reverse transcriptase (RT) and protease appeared that are associated with drug resistance in group M viruses, the observed T215N mutation in RT and the V15I and V22A mutations in protease have not previously been described and may represent resistance-conferring mutations specific to group O viruses. These results indicate that treatment of HIV-1 group O-infected individuals with antiretroviral drug regimens that include protease inhibitors might lead to rapid selection for resistance-conferring mutations. This probably results from preexisting protease residues contributing to reduced sensitivity of group O viruses to protease inhibitors, as is observed in vitro.

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The HIV-2 genotype and the HIV-1 syncytium-inducing phenotype are associated with a lower virus replication in dendritic cells

et al. 2000

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During sexual transmission, HIV infects the mucosal dendritic cells and is transferred to CD4 T cells. Whether HIV variants of a particular genetic (sub)type or phenotype selectively infect dendritic cells (DC) or are preferentially transferred to T cells remains highly controversial. To avoid the cumbersome use of primary dendritic cells, in vitro dendritic cell models were generated from precursors, either hematopoietic progenitor cells (HPC) or monocytes (MO). Productive infection in the dendritic cells and transfer of the virus to T cells was assessed for a range of HIV variants. HPC-derived dendritic cells (HPC-DC) were more susceptible to HIV-1 than to HIV-2 isolates. The HIV-1 group O strains were more productive in HPC-DC than group M, but amongst the latter, no subtype-related difference was observed. Both non-syncytium-inducing (NSI) and SI HIV isolates and lab strains could productively infect HPC-DC, albeit with a different efficiency. Adding blocking antibodies confirmed that both CCR-5 and CXCR-4 co-receptors were functional. Biological HIV-1 clones of the NSI/R5 phenotype infected more readily HPC-DC than SI/X4 clones. MO-derived dendritic cells were, however, more exclusive in their preference for NSI/R5 clones. Some HIV variants, that did not grow readily in HPC-DC alone, could be rescued by adding resting or pre-activated T cells. The present data show that HIV-2 isolates and SI clones replicate less in model-DC, but no preference for a particular HIV-1 subtype was evident. Co-culture with T cells could "correct" a limited growth in dendritic cells. Clearly, both intrinsic dendritic cell susceptibility and enhancement by T cells are explained only partly by HIV genotype and phenotype. The in vitro dendritic cell models seem useful tools to further unravel interactions between HIV, DC, and T cells.

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Virologic, immunologic, and clinical follow-up of a couple infected by the human immunodeficiency virus type one, group O

Cited by 17 publications

References 40 publications

HIV-1 Group O Genotypes and Phenotypes: Relationship to Fitness and Susceptibility to Antiretroviral Drugs

HIV-1 Group O Genotypes and Phenotypes: Relationship to Fitness and Susceptibility to Antiretroviral Drugs

Natural Residues versus Antiretroviral Drug-Selected Mutations in HIV Type 1 Group O Reverse Transcriptase and Protease Related to Virological Drug Failurein Vivo

The HIV-2 genotype and the HIV-1 syncytium-inducing phenotype are associated with a lower virus replication in dendritic cells

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