Immunogenomic profile at baseline predicts host susceptibility to clinical malaria

基线免疫基因组图谱可预测宿主对临床疟疾的易感性

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作者:Gillian Mbambo, Ankit Dwivedi, Olukemi O Ifeonu, James B Munro, Biraj Shrestha, Robin E Bromley, Theresa Hodges, Ricky S Adkins, Bourema Kouriba, Issa Diarra, Amadou Niangaly, Abdoulaye K Kone, Drissa Coulibaly, Karim Traore, Amagana Dolo, Mahamadou A Thera, Matthew B Laurens, Ogobara K Doumbo, Chri

Conclusion

This study highlights the importance of baseline immune signatures in determining disease outcome. Our data suggests that differences in apoptotic and inflammatory gene expression patterns can serve as predictive markers of susceptibility to clinical malaria.

Methods

We analyzed peripheral blood mononuclear cells (PBMCs) collected from children who differed in susceptibility to clinical malaria, all from a small town in Mali. PBMCs were collected from children aged 4-6 years at the start, peak and end of the malaria season. We characterized the immune cell composition and cytokine secretion for a subset of 20 children per timepoint (10 children with no symptomatic malaria age-matched to 10 children with >2 symptomatic malarial illnesses), and gene expression patterns for six children (three per cohort) per timepoint.

Results

We observed differences between the two groups of children in the expression of genes related to cell death and inflammation; in particular, inflammatory genes such as CXCL10 and STAT1 and apoptotic genes such as XAF1 were upregulated in susceptible children before the transmission season began. We also noted higher frequency of HLA-DR+ CD4 T cells in protected children during the peak of the malaria season and comparable levels cytokine secretion after stimulation with malaria schizonts across all three time points.

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