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A population of CD4hiCD38hi T cells correlates with disease severity in patients with acute malaria

journal contribution
posted on 2024-11-02, 17:58 authored by Simon Apte, Gabriela Minigo, Magdalena PlebanskiMagdalena Plebanski, Katie FlanaganKatie Flanagan
Objective: CD4+ T cells are critical mediators of immunity to Plasmodium spp. infection, but their characteristics during malarial episodes and immunopathology in naturally infected adults are poorly defined. Flow cytometric analysis of PBMCs from patients with either P. falciparum or P. knowlesi malaria revealed a pronounced population of CD4+ T cells co-expressing very high levels of CD4 and CD38 we have termed CD4hiCD38hi T cells. We set out to gain insight into the function of these novel cells. Methods: CD4+ T cells from 18 patients with P. falciparum or P. knowlesi malaria were assessed by flow cytometry and sorted into populations of CD4hiCD38hi or CD4norm T cells. Gene expression in the sorted populations was assessed by qPCR and NanoString. Results: CD4hiCD38hi T cells expressed high levels of CD4 mRNA and canonical type 1 regulatory T-cell (TR1) genes including IL10, IFNG, LAG3 and HAVCR2 (TIM3), and other genes with relevance to cell migration and immunomodulation. These cells increased in proportion to malaria disease severity and were absent after parasite clearance with antimalarials. Conclusion: In naturally infected adults with acute malaria, a prominent population of type 1 regulatory T cells arises that can be defined by high co-expression of CD4 and CD38 (CD4hiCD38hi) and that correlates with disease severity in patients with falciparum malaria. This study provides fundamental insights into T-cell biology, including the first evidence that CD4 expression is modulated at the mRNA level. These findings have important implications for understanding the balance between immunity and immunopathology during malaria.

Funding

Research Fellowship

National Health and Medical Research Council

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Tropical Disease - immunity, pathogenesis and vaccine development: global translation

National Health and Medical Research Council

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Tropical diseases: Translating discoveries into better health

National Health and Medical Research Council

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Pathophysiology and treatment of malaria in our region

National Health and Medical Research Council

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Risk factors, mechanisms, and treatment of knowlesi malaria

National Health and Medical Research Council

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History

Related Materials

  1. 1.
    DOI - Is published in 10.1002/cti2.1209
  2. 2.
    ISSN - Is published in 20500068

Journal

Clinical and Translational Immunology

Volume

9

Number

e1209

Issue

11

Start page

1

End page

18

Total pages

18

Publisher

John Wiley & Sons

Place published

United Kingdom

Language

English

Copyright

© 2020 The Authors. Clinical & Translational Immunology

Former Identifier

2006109952

Esploro creation date

2021-10-13

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