Malaria systems immunology: Plasmodium vivax induces tolerance during primary infection through dysregulation of neutrophils and dendritic cells - 04/10/18

Doi : 10.1016/j.jinf.2018.09.005

Andres F. Vallejo ^a, Robert C. Read ^a, Myriam Arevalo-Herrera ^b,^c, Sócrates Herrera ^b, Tim Elliott ^d,^e, Marta E. Polak ^a,^e,^⁎
^a Clinical and Experimental Sciences and NIHR Southampton Biomedical Research Centre, Faculty of Medicine, University of Southampton, Southampton General Hospital, LE59, MP813, SO16 6YD, Southampton, UK
^b Caucaseco Scientific Research Center, Cali, 760043, Colombia
^c School of Health, Universidad del Valle, Cali, 76001, Colombia
^d Centre for Cancer Immunology, Faculty of Medicine, University of Southampton, SO16 6YD Southampton, UK
^e Institute for Life Sciences, University of Southampton, SO17 1BJ, UK

^⁎Corresponding author at: Clinical and Experimental Sciences, Faculty of Medicine, University of Southampton, Southampton General Hospital, LE59, MP813, SO16 6YD Southampton, UK.Clinical and Experimental Sciences, Faculty of MedicineUniversity of Southampton,Southampton General Hospital, LE59, MP813SouthamptonSO16 6YDUK

Sous presse. Épreuves corrigées par l'auteur. Disponible en ligne depuis le Thursday 04 October 2018

Highlights

•	In silico analysis suggests that primary infection with P. vivax induces potent immunosuppression mediated by dendritic cells.
•	Antigen presentation is attenuated in malaria-experienced vs malaria-naïve individuals
•	Malaria induce immunosuppressive effect manifested with strong induction of IDO1.

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Summary

Objectives

To dissect the transcriptional networks underpinning immune cells responses during primary Plasmodium vivax infection of healthy human adults.

Methods

We conducted network co-expression analysis of next-generation RNA sequencing data from whole blood from P. vivax and P. falciparum controlled human malaria infection (CHMI) of healthy naïve and malaria-exposed volunteers. Single cell transcription signatures were used to deconvolute the bulk RNA-Seq data into cell-specific signals.

Results

Initial exposure to P. vivax induced activation of innate immunity, including efficient antigen presentation and complement activation. However, this effect was accompanied by strong immunosuppression mediated by dendritic cells via the induction of Indoleamine 2,3-Dioxygenase 1(IDO1) and Lymphocyte Activation Gene 3 (LAG3). Additionally, P. vivax induced depletion of neutrophil populations associated with down regulation of 3G-protein coupled receptors, CRXCR1, CXCR2 and CSF3R. Accordingly, in malaria-exposed volunteers the inflammatory response was attenuated, with a decreased class II antigen presentation in dendritic cells. While the immunosuppressive signalling was maintained between plasmodium species, response to P. falciparum was significantly more immunogenic.

Conclusions

In silico analyses suggest that primary infection with P. vivax induces potent immunosuppression mediated by dendritic cells, conditioning subsequent anti-malarial immune responses. Targeting immune evasion mechanisms could be an effective alternative for improving vaccine efficacy.

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Keywords : Malaria, Controlled human malaria infection, Transcriptomics, Dendritic cells, Immunoregulation, Vaccines