Cytotoxic T lymphocyte activity and CD8 subpopulations in children at risk of HIV infection

Aldhous, Marian C.; Watret, Karen C.; Mok, Jacqueline; Bird, A. G.; Froebel, K. S.

doi:10.1111/j.1365-2249.1994.tb06580.x

Cited by 46 publications

(8 citation statements)

References 35 publications

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“…We found that 45% of infants were able to generate cellular immune responses of substantial breadth and magnitude; however, most responses were transient. Our finding confirms previous studies that detected responses in HIV-1 EU infants [22,27,28,31], and is consistent with our previous study that observed 47% prevalence of at least one positive ELISPOT assay using human leucocyte antigen (HLA)-matched peptide stimulation in breastfeeding EU infants [29]. We also found significant associations between maternal plasma and breastmilk HIV-1 viral levels and infant magnitude of HIV-1-specific ELISPOT responses, suggesting that antigen exposure modifies the induced infant HIV-1-specific immune responses.…”

Section: Discussionsupporting

confidence: 93%

“…HIV-1-specific cellular immune responses have been reported in varied HIV-1 EU populations, including commercial sex workers [15][16][17], HIV-1-discordant couples [18][19][20] and infants born to HIV-1-infected women [21][22][23]. CD4 1 and CD8 1 HIV-1-specific responses have been observed in EU infants, with prevalence ranging from 3 to 56% [24][25][26][27] and 0 to 47% [22,[27][28][29][30][31], respectively, resulting in controversy around the detection of these responses and their potential protective role. However, vaccine development relies upon understanding the induction of immune responses, and so it remains important to identify the correlates of presence and magnitude of HIV-1specific immune responses in EU individuals.…”

Section: Introductionmentioning

confidence: 99%

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Maternal plasma and breastmilk viral loads are associated with HIV-1-specific cellular immune responses among HIV-1-exposed, uninfected infants in Kenya

Liu

Lohman-Payne

Chung

et al. 2015

Clinical and Experimental Immunology

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SummaryInfants exposed to maternal HIV-1 provide an opportunity to assess correlates of HIV-1-specific interferon ( Maternal plasma HIV-1 RNA levels during pregnancy (P 5 0Á009) and breastmilk HIV-1 DNA levels at 1 month (P 5 0Á02) were associated with a higher magnitude of infant HIV-1-specific ELISPOT responses at 1 month postpartum. During follow-up, concurrent breastmilk HIV-1 RNA and DNA (cell-free virus and cell-associated virus, respectively) each were associated positively with magnitude of infant HIV-1-specific responses (P 5 0Á01). Our data demonstrate the importance of antigenic exposure on the induction of infant HIV-1-specific cellular immune responses in the absence of infection.

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Section: Discussionsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Maternal plasma and breastmilk viral loads are associated with HIV-1-specific cellular immune responses among HIV-1-exposed, uninfected infants in Kenya

Liu

Lohman-Payne

Chung

et al. 2015

Clinical and Experimental Immunology

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“…Previous studies by our group and others in perinatal HIV-exposed infants have reported evidence of HIV-specific immune response (4,(18)(19)(20)(21)(22)(23)(24)(25). HIV-specific immune response has also been observed in exposed noninfected adults (26)(27)(28)(29).…”

Section: Discussionsupporting

confidence: 57%

Imbalance of naive and memory T lymphocytes with sustained high cellular activation during the first year of life from uninfected children born to HIV-1-infected mothers on HAART

Ono

Santos

Succi

et al. 2008

Braz J Med Biol Res

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The immune consequences of in utero HIV exposure to uninfected children whose mothers were submitted to highly active antiretroviral therapy (HAART) during gestation are not well defined. We evaluated 45 HIV-exposed uninfected (ENI) neonates and 45 healthy unexposed control (CT) neonates. All HIV-infected mothers received HAART during pregnancy, and the viral load at delivery was <50 copies/mL for 56.8%. Twenty-three ENI neonates were further evaluated after 12 months and compared to 23 unexposed healthy age-matched infants. Immunophenotyping was performed by flow cytometry in cord and peripheral blood. Cord blood lymphocyte numbers did not differ between groups. However, ENI neonates had a lower percentage of naive T cells than CT neonates (CD4+, 76.6 vs 83.1%, P < 0.001; CD8+, 70.9 vs 79.6%, P = 0.003) and higher percentages of central memory T cells than CT neonates (CD4+, 13.9 vs 8.7%, P < 0.001; CD8+, 8.6 vs 4.8%, P = 0.001). CD38 mean fluorescence intensity of T cells was higher in ENI neonates (CD4+, 62.2 vs 52.1, P = 0.007; CD8+, 47.7 vs 35.3, P < 0.001). At 12 months, ENI infants still had higher mean fluorescence intensity of CD38 on T cells (CD4+, 34.2 vs 23.3, P < 0.001; CD8+, 26.8 vs 19.4, P = 0.035). Despite effective maternal virologic control at delivery, HIV-exposed uninfected children were born with lower levels of naive T cells. Immune activation was present at birth and remained until at least 12 months of age, suggesting that in utero exposure to HIV causes subtle immune abnormalities.

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“…However, in the study by Betts et al, variations in the number of HIVspecific CD8 + T-cell in chronically infected patients were in much broader ranges -between 1.6 and 18.4% of total CD8 + T-cells [83]. HIV-1-specific CD8 + CTLs in HIV-1-infected children have frequency and specificity similar to those found in HIV-1-infected adults [84][85][86]. Frequencies of SIV-and HIV-1-specific T-cells are not the sole determinants of immunemediated protection in viral infection [83].…”

mentioning

confidence: 85%

Peptide–MHC multimer-based monitoring of CD8 T-cells in HIV-1 infection and AIDS vaccine development

Reguzova

Karpenko

Mechetina

et al. 2014

Expert Review of Vaccines

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The use of MHC multimers allows precise and direct detecting and analyzing of antigen-specific T-cell populations and provides new opportunities to characterize T-cell responses in humans and animals. MHC-multimers enable us to enumerate specific T-cells targeting to viral, tumor and vaccine antigens with exceptional sensitivity and specificity. In the field of HIV/SIV immunology, this technique provides valuable information about the frequencies of HIV- and SIV-specific CD8(+) cytotoxic T lymphocytes (CTLs) in different tissues and sites of infection, AIDS progression, and pathogenesis. Peptide-MHC multimer technology remains a very sensitive tool in detecting virus-specific T -cells for evaluation of the immunogenicity of vaccines against HIV-1 in preclinical trials. Moreover, it helps to understand how immune responses are formed following vaccination in the dynamics from priming point until T-cell memory is matured. Here we review a diversity of peptide-MHC class I multimer applications for fundamental immunological studies in different aspects of HIV/SIV infection and vaccine development.

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Cytotoxic T lymphocyte activity and CD8 subpopulations in children at risk of HIV infection

Cited by 46 publications

References 35 publications

Maternal plasma and breastmilk viral loads are associated with HIV-1-specific cellular immune responses among HIV-1-exposed, uninfected infants in Kenya

Maternal plasma and breastmilk viral loads are associated with HIV-1-specific cellular immune responses among HIV-1-exposed, uninfected infants in Kenya

Imbalance of naive and memory T lymphocytes with sustained high cellular activation during the first year of life from uninfected children born to HIV-1-infected mothers on HAART

Peptide–MHC multimer-based monitoring of CD8 T-cells in HIV-1 infection and AIDS vaccine development

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