T-cell immunity to peptide epitopes of liver-stage antigen 1 in an area of Papua New Guinea in which malaria is holoendemic

Connelly, Marc; King, Christopher L.; Bucci, Kim; Walters, S.; Genton, Blaise; Alpers, Michael P.; Hollingdale, Michael R.; Kazura, James W.

doi:10.1128/iai.65.12.5082-5087.1997

Cited by 61 publications

(20 citation statements)

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“…Immunization of mice with HEP17 plasmid DNA induced CD8 þ T cells against a yet to be identified epitope in the protein (36). Further studies on TRAP/SSP2 and HEP17/ EXP1 have been severely hampered by the failure to identify putative epitopes recognized by protective CD8 þ T cells (37)(38)(39)(40)(41)(42)(43)(44)(45)(46).…”

Section: Introductionmentioning

confidence: 99%

Effector and memory CD8⁺ T cells as seen in immunity to malaria

Morrot

Zavala

2004

Immunological Reviews

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Transgenic (Tg) mice carrying a T-cell receptor (TCR) specific for a CD8(+) T-cell epitope expressed in pre-erythrocytic stages of Plasmodium yoelii has proven to be a valuable tool to advance our understanding of this anti-parasite T-cell response, as it occurs in vivo. The visualization of CD8(+) T cells in vivo and ex vivo greatly facilitated research aimed at characterizing basic features of this T-cell response such as the kinetics of differentiation and proliferation and the in vivo antigen presentation. Importantly, this research unveiled the existence of early self-regulatory mechanisms controlling the magnitude of the CD8(+) T-cell response and also identified CD4(+) T cells as critical elements in the development of memory populations. This review discusses our recent research using Tg mice and highlights our progress in understanding the CD8(+) T-cell-mediated immunity against malaria liver stages.

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Section: Introductionmentioning

confidence: 99%

Effector and memory CD8⁺ T cells as seen in immunity to malaria

Morrot

Zavala

2004

Immunological Reviews

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“…Recent studies conducted in Kenya and Gabon indicate that cytokine responses to N-and C-terminal non-repeat regions of LSA-1 correlate with partial resistance to re-infection [13±15]. Using a consensus sequence based on the NF54 P. falciparum isolate, we previously characterized T cell cytokine responses to peptides encoded by LSA-1 amino acid residues 84±107, 1813±1835, and 1888±1909 in adults living in the Wosera area of East Sepik Province, Papua New Guinea [16]. Whereas only 18% of individuals had IL-4 or IL-5 responses, IFN-g production stimulated by the N-terminal 84±107 peptide was observed in 33% of the subjects.…”

Section: Introductionmentioning

confidence: 99%

Influence of age and HLA type on interferon-gamma (IFN-γ) responses to a naturally occurring polymorphic epitope ofPlasmodium falciparumliver stage antigen-1 (LSA-1)

Bucci

Kastens

Hollingdale

et al. 2000

Clinical and Experimental Immunology

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SUMMARYAntigenic polymorphism and HLA restriction may limit the immunogenicity of a subunit vaccine against liver-stage Plasmodium falciparum. We examined 59 clinical isolates and five laboratory clones of P. falciparum for polymorphism in the N-and C-terminal regions of LSA-1, evaluated binding of the corresponding peptides to selected HLA class I alleles, and measured IFN-g responses in residents of a malaria-endemic area of Papua New Guinea where HLA-A*1101, -24, -B13, and -B40 are the most common class I alleles. LSA-1 polymorphism was limited to a single non-synonymous mutation encoding serine (S), proline (P), or threonine (T) at amino acid 85. Nine-mer 84±92 peptides with S, T, or P at the primary anchor position bound differentially to HLA-A11, -A2, and -B7. IFN-g ELISPOT responses increased with age in malaria-exposed subjects: 14±16% and 30±36% of 2±5-and 6±54-yearolds, respectively, had $ 10 IFN-g-secreting cells/10 6 peripheral blood mononuclear cells when stimulated with at least one peptide variant (P , 0´05). IFN-g responses to all three peptides were also greater for older than younger individuals. No children , 3 years old had lymphocytes that responded to all three 84±92 peptides, whereas 45% of adults (mean age 48 years) had aggregated IFN-g responses. These data support the notion that age-related cumulative exposure to P. falciparum increases the frequency of IFN-g responses to polymorphic epitopes of liver-stage antigens such as LSA-1.

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“…Human studies have identified low levels of CTL activity in naturally exposed populations (1,10,16,22) and in irradiated sporozoite-immunized volunteers (24,33). Other studies indicate that antibody, proliferative, cytokine, and CTL responses to LSA-1 peptides are detectable in naturally exposed individuals (8,11,12). Connelly et al reported that in an area of Papua New Guinea where malaria is holoendemic, 10 of 11 individuals with two negative blood smears (obtained 6 months apart) produced detectable IFN-␥ in response to an LSA-1 peptide, while only 9 of 27 individuals with one or two positive blood smears produced detectable IFN-␥ in response to this peptide (8).…”

Section: Discussionmentioning

confidence: 98%

“…Other studies indicate that antibody, proliferative, cytokine, and CTL responses to LSA-1 peptides are detectable in naturally exposed individuals (8,11,12). Connelly et al reported that in an area of Papua New Guinea where malaria is holoendemic, 10 of 11 individuals with two negative blood smears (obtained 6 months apart) produced detectable IFN-␥ in response to an LSA-1 peptide, while only 9 of 27 individuals with one or two positive blood smears produced detectable IFN-␥ in response to this peptide (8). No association was found between blood smear status and IFN-␥ responses to two other LSA-1 peptides.…”

Section: Discussionmentioning

confidence: 98%

Interleukin-10 Responses to Liver-Stage Antigen 1 Predict Human Resistance toPlasmodium falciparum

et al. 1999

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The design of an effective vaccine against Plasmodium falciparum, the most deadly malaria parasite of humans, requires a careful definition of the epitopes and the immune responses involved in protection. Liver-stage antigen 1 (LSA-1) is specifically expressed during the hepatic stage of P. falciparum and elicits cellular and humoral immune responses in naturally exposed individuals. We report here that interleukin-10 (IL-10) production in response to LSA-1 predicts resistance to P. falciparum after eradication therapy. Resistance was not related to gamma interferon or tumor necrosis factor alpha production. This is the first report that human IL-10 responses are associated with resistance after eradication therapy, and our findings support the inclusion of LSA-1 in a vaccine against malaria.

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T-cell immunity to peptide epitopes of liver-stage antigen 1 in an area of Papua New Guinea in which malaria is holoendemic

Cited by 61 publications

References 32 publications

Effector and memory CD8⁺ T cells as seen in immunity to malaria

Effector and memory CD8⁺ T cells as seen in immunity to malaria

Influence of age and HLA type on interferon-gamma (IFN-γ) responses to a naturally occurring polymorphic epitope ofPlasmodium falciparumliver stage antigen-1 (LSA-1)

Interleukin-10 Responses to Liver-Stage Antigen 1 Predict Human Resistance toPlasmodium falciparum

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T-cell immunity to peptide epitopes of liver-stage antigen 1 in an area of Papua New Guinea in which malaria is holoendemic

Cited by 61 publications

References 32 publications

Effector and memory CD8+ T cells as seen in immunity to malaria

Effector and memory CD8+ T cells as seen in immunity to malaria

Influence of age and HLA type on interferon-gamma (IFN-γ) responses to a naturally occurring polymorphic epitope ofPlasmodium falciparumliver stage antigen-1 (LSA-1)

Interleukin-10 Responses to Liver-Stage Antigen 1 Predict Human Resistance toPlasmodium falciparum

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Effector and memory CD8⁺ T cells as seen in immunity to malaria

Effector and memory CD8⁺ T cells as seen in immunity to malaria