Quantification of naive and memory T-cell turnover during HIV-1 infection

Vrisekoop, Nienke; Drylewicz, Julia; Gent, Rogier van; Mugwagwa, Tendai; Lelyveld, S.F.L. van; Veel, Ellen; Otto, Sigrid A.; Ackermans, Mariëtte T.; Vermeulen, Joost N.; Huidekoper, Hidde H.; Prins, Jan M.; Miedema, Frank; Boer, Rob J. de; Tesselaar, Kiki; Borghans, José A. M.

doi:10.1097/qad.0000000000000822

Cited by 28 publications

(40 citation statements)

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“…A large variety of techniques, varying from Ki67 staining [37, 71, 193, 247], BrdU labeling [46, 121, 132, 162], deuterium labeling [103, 105, 134, 163, 224], TREC analysis [60, 62, 102, 140, 187], telomere analysis [173, 238, 239] and various combinations thereof [61, 89, 172] have unequivocally established that T lymphocytes are turning over more rapidly in chronically infected patients and macaques than in healthy controls. It has been difficult to precisely quantify the fold increase in T lymphocyte turnover because (1) the estimation of turnover rates from this data can be challenging, (2) studies have not always separated naive from memory T cells, and (3) the rates of cell division, i.e., the fraction of Ki67 + T cells, depend on the viral load and the density of CD4 + T cells [37, 193].…”

Section: Discussionmentioning

confidence: 99%

“…It has been difficult to precisely quantify the fold increase in T lymphocyte turnover because (1) the estimation of turnover rates from this data can be challenging, (2) studies have not always separated naive from memory T cells, and (3) the rates of cell division, i.e., the fraction of Ki67 + T cells, depend on the viral load and the density of CD4 + T cells [37, 193]. Long-term deuterium labeling in volunteers and HIV-1 infected patients suggests that the turnover rate of memory CD4 + and CD8 + T cells is approximately 3-fold increased in patients with CD4 + T cell counts between 180 to 450 cells per μ l blood [224]. The variation in the turnover rate of naive T cells was higher, with a similar 3-fold increase in the naive CD4 + T cell compartment, and a 12-fold increase for CD8 + naive T cells [224].…”

Section: Discussionmentioning

confidence: 99%

“…We recently found that these labeling data from human naive T cells are well described by the single compartment version of Eq. (21), arguing that human naive T cells form a homogeneous population of long-lived cells [224]. However, the data from the memory T cells in that study [223] required at least two compartments to obtain a good fit to the labeling data, suggesting that memory T cells form a heterogeneous population [231].…”

Section: Dna Labeling Techniquesmentioning

confidence: 99%

“…Estimates of the death rate are available from studies using deuterium labeling of CD4 + naive T cells in healthy volunteers [223] and HIV + patients [224], which suggested average loss rates of d = 0.0005 day −1 and d = 0.00152 day −1 , respectively (i.e., life spans of 5.6 and 1.8 years, respectively; just exceeding a 3-fold difference). Naive T cell counts are depleted during HIV-1 infection, and after one or two years of HIV-1 infection one readily observes a 5-fold TREC dilution and a 2-fold reduction of the number of naive CD4 + T cells in the blood.…”

Section: Trecs and Telomeresmentioning

confidence: 99%

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Quantifying T lymphocyte turnover

Boer

Perelson

2013

Journal of Theoretical Biology

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Peripheral T cell populations are maintained by production of naive T cells in the thymus, clonal expansion of activated cells, cellular self-renewal (or homeostatic proliferation), and density dependent cell life spans. A variety of experimental techniques have been employed to quantify the relative contributions of these processes. In modern studies lymphocytes are typically labeled with 5-bromo-2′-deoxyuridine (BrdU), deuterium, or the fluorescent dye carboxy-fluorescein diacetate succinimidyl ester (CFSE), their division history has been studied by monitoring telomere shortening and the dilution of T cell receptor excision circles (TRECs) or the dye CFSE, and clonal expansion has been documented by recording changes in the population densities of antigen specific cells. Proper interpretation of such data in terms of the underlying rates of T cell production, division, and death has proven to be notoriously difficult and involves mathematical modeling. We review the various models that have been developed for each of these techniques, discuss which models seem most appropriate for what type of data, reveal open problems that require better models, and pinpoint how the assumptions underlying a mathematical model may influence the interpretation of data. Elaborating various successful cases where modeling has delivered new insights in T cell population dynamics, this review provides quantitative estimates of several processes involved in the maintenance of naive and memory, CD4+ and CD8+ T cell pools in mice and men.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Dna Labeling Techniquesmentioning

confidence: 99%

Section: Trecs and Telomeresmentioning

confidence: 99%

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Quantifying T lymphocyte turnover

Boer

Perelson

2013

Journal of Theoretical Biology

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215

275

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“…X4-R5 reversions have already been reported in HIV-1-infected patients after immune reconstitution [51–54]. Because recent findings indicate that X4-capable HIV-1 viruses are less susceptible to neutralization by autologous antibodies than R5-using viruses from the same host [55], X4-R5 reversions could result from the normalization of naïve T-cell turnover following immunological recovery [56], after which the infection of naïve T-cells by X4-capable variants may not be productive enough [51]. Since X4-capable HIV-2 also seem to be less susceptible to neutralization than CCR5-using strains [19], X4-R5 reversions in HIV-2 could be explained by the same mechanism.…”

Section: Discussionmentioning

confidence: 99%

A genotypic method for determining HIV-2 coreceptor usage enables epidemiological studies and clinical decision support

et al. 2016

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BackgroundCCR5-coreceptor antagonists can be used for treating HIV-2 infected individuals. Before initiating treatment with coreceptor antagonists, viral coreceptor usage should be determined to ensure that the virus can use only the CCR5 coreceptor (R5) and cannot evade the drug by using the CXCR4 coreceptor (X4-capable). However, until now, no online tool for the genotypic identification of HIV-2 coreceptor usage had been available. Furthermore, there is a lack of knowledge on the determinants of HIV-2 coreceptor usage. Therefore, we developed a data-driven web service for the prediction of HIV-2 coreceptor usage from the V3 loop of the HIV-2 glycoprotein and used the tool to identify novel discriminatory features of X4-capable variants.ResultsUsing 10 runs of tenfold cross validation, we selected a linear support vector machine (SVM) as the model for geno2pheno[coreceptor-hiv2], because it outperformed the other SVMs with an area under the ROC curve (AUC) of 0.95. We found that SVMs were highly accurate in identifying HIV-2 coreceptor usage, attaining sensitivities of 73.5% and specificities of 96% during tenfold nested cross validation. The predictive performance of SVMs was not significantly different (p value 0.37) from an existing rules-based approach. Moreover, geno2pheno[coreceptor-hiv2] achieved a predictive accuracy of 100% and outperformed the existing approach on an independent data set containing nine new isolates with corresponding phenotypic measurements of coreceptor usage. geno2pheno[coreceptor-hiv2] could not only reproduce the established markers of CXCR4-usage, but also revealed novel markers: the substitutions 27K, 15G, and 8S were significantly predictive of CXCR4 usage. Furthermore, SVMs trained on the amino-acid sequences of the V1 and V2 loops were also quite accurate in predicting coreceptor usage (AUCs of 0.84 and 0.65, respectively).ConclusionsIn this study, we developed geno2pheno[coreceptor-hiv2], the first online tool for the prediction of HIV-2 coreceptor usage from the V3 loop. Using our method, we identified novel amino-acid markers of X4-capable variants in the V3 loop and found that HIV-2 coreceptor usage is also influenced by the V1/V2 region. The tool can aid clinicians in deciding whether coreceptor antagonists such as maraviroc are a treatment option and enables epidemiological studies investigating HIV-2 coreceptor usage. geno2pheno[coreceptor-hiv2] is freely available at http://coreceptor-hiv2.geno2pheno.org.Electronic supplementary materialThe online version of this article (doi:10.1186/s12977-016-0320-7) contains supplementary material, which is available to authorized users.

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