| Literature DB >> 26471813 |
Charlotte Joos1,2, Marie-Louise Varela3, Babacar Mbengue4, Annick Mansourou5, Laurence Marrama6, Cheikh Sokhna7, Adama Tall8, Jean-François Trape9, Aissatou Touré10, Odile Mercereau-Puijalon11, Ronald Perraut12.
Abstract
BACKGROUND: Identification of plasmodial antigens targeted by protective immune mechanisms is important for malaria vaccine development. Among functional assays, the neutrophil antibody-dependent respiratory burst (ADRB) induced by opsonized Plasmodium falciparum merozoites has been correlated with acquired immunity to clinical malaria in endemic areas, but the target merozoite antigens are unknown. Here, the contribution of antibodies to the conserved C-terminal domain of the P. falciparum merozoite surface protein-1 (PfMSP1p19) in mediating ADRB was investigated in sera from individuals living in two Senegalese villages with differing malaria endemicity.Entities:
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Year: 2015 PMID: 26471813 PMCID: PMC4608189 DOI: 10.1186/s12936-015-0935-5
Source DB: PubMed Journal: Malar J ISSN: 1475-2875 Impact factor: 2.979
Antibody responses against MSP1p19 in Dielmo and Ndiop villagers tested for ADRB
| Age groups (years) | N | Mean age (years) | Anti-PfMSP1p19 levelsa | % Positive respondersb | % High respondersb | ADRBc |
|---|---|---|---|---|---|---|
| DIELMO | ||||||
| 0–6 | 19 | 4.6 | 3.6 [1–9.1] | 68 | 16 | 154 [46–354] |
| 7–14 | 31 | 10.9 | 3.5 [1–15] | 48 | 13 | 231 [40–958] |
| ≥15 | 69 | 37.4 | 9.2 [1–16.9] | 87 | 62 | 380 [106–575] |
| All | 119 | 25.3 | 6.8 [1–16.9] | 74 | 42 | 305 [40–958] |
| NDIOP | ||||||
| 0–14 | 49 | 8.8 | 6.4 [1–18.4] | 80 | 37 | 162 [51–545] |
| 15–29 | 33 | 20.5 | 9.2 [1–19.7] | 88 | 55 | 307 [113–1721] |
| ≥30 | 32 | 43.9 | 11.9 [1–19.9] | 94 | 69 | 370 [56–1147] |
| All | 114 | 21.8 | 8.8 [1–19.9] | 86 | 51 | 262 [51–1721] |
aMean [range] antibody levels to PfMSP1p19 expressed in OD-ratio
bPercent of responders (OD-ratio > 2) and of High responders (OD-ratio > 7)
cMean level and range [min–max] of ADRB measured in villagers’ sera
Fig. 1ADRB responses stratified by anti PfMSP1p19 antibody levels in the two villages. ADRB measured in 119 and 114 sera from Dielmo and Ndiop, respectively are plotted as function of their anti-PfMSP1p19 antibodies responses stratified into three levels: non-responders (NR), positive responders (PR, OD ratio > 2) and strong responders (SR, OD ratio > 7). The SR level was selected according to previous study [21] underlining this critical threshold of antibody levels to PfMSP1p19 in Ndiop. Boxplot graphs show that the profile of ADRB responses strongly and significantly increase (P < 10−3) with increasing anti-PfMSP1p19 antibodies content. The median is indicated by a line, the 50 % percentiles indicated by the box limits and the upper and lower 25 % by whiskers
Fig. 2Naturally-acquired anti-PfMSP1p19 antibodies are major inducers of ADRB activity against P. falciparum merozoites. a ADRB chemiluminescence readout for 21 sera with high anti-PfMSP1p19 OD-ratios tested using either P. falciparum D10 merozoites (D10-PfM3′, black bars) or transgenic D10 merozoites in which the P. falciparum MSP1p19 gene was replaced by its P. chabaudi orthologue (D10-PcMEGF, black bars). D10-PfM3′ and D10-PcMEGF merozoites were tested in the same plate, with the same polymorphonuclear cells batch. b Boxplot graph showing the significant (P < 10−3) overall distribution of ADRB generated using sera and D10-PfM3′ or D10-PcMEGF transgenic merozoites. The median is indicated by a line, the 50 % percentiles indicated by the box limits and the upper and lower 25 % by whiskers
Fig. 3Effect of anti-PfMSP1p19 depletion on ADRB activity against P. falciparum merozoites. A set of 21 sera were depleted from anti-PfMSP1p19 antibodies using metal affinity immuno-adsorbent. a The ADRB level of each serum pair (undepleted and depleted, black and light bars, respectively) was plotted in increasing order of ADRB level of undepleted sera. b Boxplot graph showing the significant (P < 10−3) overall drop of ADRB from initial vs depleted sera. All sera selected had initial high levels of anti-PfMSP1p19 antibodies. The median is indicated by a line, the 50 % percentiles indicated by the box limits and the upper and lower 25 % by whiskers
Fig. 4ADRB activity of a set of 24 sera in the solid-phase assay using PfMSP1p19-coated plates. Histograms of ADRB activity measured using PfMSP1p19-coated in 9, 11 and 4 sera from Ndiop (light grey), Dielmo (medium grey) and urban malaria (dark grey), respectively, plotted in increasing order of ADRB units, respectively. The sera were chosen irrespective of their level of antibodies to PfMSP1p19 antigen