Human Cytomegalovirus Proteins pp65 and Immediate Early Protein 1 Are Common Targets for CD8+ T Cell Responses in Children with Congenital or Postnatal Human Cytomegalovirus Infection

Gibson, Laura; Piccinini, Giampiero; Lilleri, Daniele; Revello, Maria Grazia; Wang, Zhongde; Markel, Susan; Diamond, Don J.; Luzuriaga, Katherine

doi:10.4049/jimmunol.172.4.2256

Cited by 104 publications

(80 citation statements)

References 66 publications

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“…Within the numerous antigens recognized by memory CD8+ T cells of healthy HCMVseropositive donors tested with various HLA haplotypes, IE1 and pp65 were the most immunodominant, conWrming observations claimed by several groups for many years. Moreover, CTL detected in young infants with HCMV infection were directed at both IE1 and pp65 and their appearance correlated with decrease in viral load [21,22]. This supports the notion that immunodominance could be governed by antigenic dominance, reXecting antigen amounts available at the right time when immunoevasins are not yet eVective.…”

Section: T Cell Repertoire Against Hcmv Exhibits a Broad Pattern Of Ssupporting

confidence: 66%

Interplay between human cytomegalovirus and dendritic cells in T cell activation

Martin

Mandron

Davrinche

2008

Med Microbiol Immunol

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Control of human cytomegalovirus (HCMV) infection and prevention of associated diseases in immunocompetent hosts are ensured mainly by CD8+ T cells, in spite of numerous viral tricks to impair antigen presentation and activation of T cells. At sites of primary infection, dendritic cells (DCs) are in the forefront to ensure capture of viral antigens and their capacity to bypass the eVects of viral immunoevasins is crucial in moulding CD8+ T cell repertoire. In HCMV-seropositive donors, the spectrum of CD8+ T cells speciWcities was shown to include immediate-early (IE), early (E) and late (L) gene products, a surprising Wnding if we consider that expression of immunoevasins could paralyse infected DCs from the IE phase of infection. In the present report, we suggest that uninfected dendritic cells could acquire HCMV-antigens derived from input virus or neosynthesis, either in soluble forms or in association with infected dead cells resulting from death-ligand-mediated apoptosis and necrosis. Activation of naïve CD8+ T cells could then occur in lymph nodes through cross-presentation by antigen-loaded DCs, providing an explanation for shape and size of the memory compartment.

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Section: T Cell Repertoire Against Hcmv Exhibits a Broad Pattern Of Ssupporting

confidence: 66%

Interplay between human cytomegalovirus and dendritic cells in T cell activation

Martin

Mandron

Davrinche

2008

Med Microbiol Immunol

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“…Thus, it seems that the determination of IE-and pp65-specific CD8 + T cells may in some cases underestimate the real efficiency of the immune system against HCMV infection. In this respect, it seems important to recall that changes in the protein and epitope specificity of HCMVspecific CD8 + T cells over time have been reported in children with congenital or postnatal HCMV infection [18] as well as during Epstein-Barr virus infection [19]. This might be due to different viral antigen processing and presentation [20].…”

Section: Discussionmentioning

confidence: 99%

Simultaneous quantification of human cytomegalovirus (HCMV)-specific CD4+ and CD8+T cells by a novel method using monocyte-derived HCMV-infected immature dendritic cells

et al. 2005

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Immature dendritic cells (DC) infected with an endotheliotropic (Huv + ) and leukotropic (Leuk + ) human cytomegalovirus (HCMV) strain were used as a stimulus to determine functional HCMV-specific CD4 + and CD8 + T cells. Infected DC were cocultured with autologous peripheral blood mononuclear cells and both arms of T cell activation were determined by intracellular flow cytometry analysis of IFN-c production. Efficient stimulation of HCMV-specific CD4 + and CD8 + T cell responses was achieved using DC productively infected with Huv + Leuk + VR1814 strain. On the contrary, a negligible CD8 + T cell response was obtained when HCMV strains unable to infect DC, or DC pulsed with inactivated viral antigen, were used. HCMV specificity of the T cell response was confirmed in 46 HCMV-seropositive and 8 HCMV-seronegative healthy subjects. A cut-off was established to discriminate between immune and nonimmune subjects. The novel ex vivo assay enables the simultaneous evaluation of HCMV-specific CD4 + and CD8 + T cell responses and may be a useful tool for monitoring HCMV-specific T cell activity in immunocompromised transplanted patients.

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“…Longitudinal samples were collected from young infants with ages ranging from 1 wk to 2.5 y. Prior reports from our group (63)(64)(65) and others (66) have shown that HCMV-specific CD8 + T-cell responses with similar antigen specificity, phenotype, and functional profiles as adults are detectable in infants with congenital CMV infection, even during gestation. Other studies have shown that infants can generate HIV-specific CD8 + T-cell responses that exert selective pressure and contribute to the evolution of viral quasi-species over the first year of life (67).…”

Section: Discussionmentioning

confidence: 99%

Limits and patterns of cytomegalovirus genomic diversity in humans

Renzette

Pokalyuk

Gibson

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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129

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Human cytomegalovirus (HCMV) exhibits surprisingly high genomic diversity during natural infection although little is known about the limits or patterns of HCMV diversity among humans. To address this deficiency, we analyzed genomic diversity among congenitally infected infants. We show that there is an upper limit to HCMV genomic diversity in these patient samples, with ∼25% of the genome being devoid of polymorphisms. These low diversity regions were distributed across 26 loci that were preferentially located in DNA-processing genes. Furthermore, by developing, to our knowledge, the first genome-wide mutation and recombination rate maps for HCMV, we show that genomic diversity is positively correlated with these two rates. In contrast, median levels of viral genomic diversity did not vary between putatively single or mixed strain infections. We also provide evidence that HCMV populations isolated from vascular compartments of hosts from different continents are genetically similar and that polymorphisms in glycoproteins and regulatory proteins are enriched in these viral populations. This analysis provides the most highly detailed map of HCMV genomic diversity in human hosts to date and informs our understanding of the distribution of HCMV genomic diversity within human hosts.human cytomegalovirus | HCMV | congenital CMV | virology | evolution

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Human Cytomegalovirus Proteins pp65 and Immediate Early Protein 1 Are Common Targets for CD8+ T Cell Responses in Children with Congenital or Postnatal Human Cytomegalovirus Infection

Cited by 104 publications

References 66 publications

Interplay between human cytomegalovirus and dendritic cells in T cell activation

Interplay between human cytomegalovirus and dendritic cells in T cell activation

Simultaneous quantification of human cytomegalovirus (HCMV)-specific CD4+ and CD8+T cells by a novel method using monocyte-derived HCMV-infected immature dendritic cells

Limits and patterns of cytomegalovirus genomic diversity in humans

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