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IL-17 signalling is critical for controlling subcutaneous adipose tissue dynamics and parasite burden during chronic murine Trypanosoma brucei infection

Author

Listed:
  • Matthew C. Sinton

    (University of Glasgow
    University of Glasgow
    University of Manchester)

  • Praveena R. G. Chandrasegaran

    (University of Glasgow
    University of Glasgow)

  • Paul Capewell

    (University of Glasgow
    University of Glasgow)

  • Anneli Cooper

    (University of Glasgow
    University of Glasgow)

  • Alex Girard

    (University of Glasgow
    University of Glasgow)

  • John Ogunsola

    (University of Glasgow
    University of Glasgow)

  • Georgia Perona-Wright

    (University of Glasgow
    University of Glasgow)

  • Dieudonné M Ngoyi

    (National Institute of Biomedical Research
    Member of TrypanoGEN)

  • Nono Kuispond

    (National Institute of Biomedical Research
    Member of TrypanoGEN)

  • Bruno Bucheton

    (Member of TrypanoGEN
    Institut de Recherche pour le Développement, Unité Mixte de Recherche IRD-CIRAD 177, Campus International de Baillarguet)

  • Mamadou Camara

    (Member of TrypanoGEN
    Programme National de Lutte contre la Trypanosomiase Humaine Africaine, Ministère de la Santé)

  • Shingo Kajimura

    (Beth Israel Deaconess Medical Center and Harvard Medical School
    Howard Hughes Medical Institute)

  • Cécile Bénézech

    (University of Edinburgh)

  • Neil A. Mabbott

    (University of Edinburgh)

  • Annette MacLeod

    (University of Glasgow
    University of Glasgow
    University of Glasgow
    Member of TrypanoGEN)

  • Juan F. Quintana

    (University of Glasgow
    University of Glasgow
    University of Manchester
    University of Manchester)

Abstract

In the skin, Trypanosoma brucei colonises the subcutaneous white adipose tissue, and is proposed to be competent for forward transmission. The interaction between parasites, adipose tissue, and the local immune system is likely to drive the adipose tissue wasting and weight loss observed in cattle and humans infected with T. brucei. However, mechanistically, events leading to subcutaneous white adipose tissue wasting are not fully understood. Here, using several complementary approaches, including mass cytometry by time of flight, bulk and single cell transcriptomics, and in vivo genetic models, we show that T. brucei infection drives local expansion of several IL-17A-producing cells in the murine WAT, including TH17 and Vγ6+ cells. We also show that global IL-17 deficiency, or deletion of the adipocyte IL-17 receptor protect from infection-induced WAT wasting and weight loss. Unexpectedly, we find that abrogation of adipocyte IL-17 signalling results in a significant accumulation of Dpp4+ Pi16+ interstitial preadipocytes and increased extravascular parasites in the WAT, highlighting a critical role for IL-17 signalling in controlling preadipocyte fate, subcutaneous WAT dynamics, and local parasite burden. Taken together, our study highlights the central role of adipocyte IL-17 signalling in controlling WAT responses to infection, suggesting that adipocytes are critical coordinators of tissue dynamics and immune responses to T. brucei infection.

Suggested Citation

  • Matthew C. Sinton & Praveena R. G. Chandrasegaran & Paul Capewell & Anneli Cooper & Alex Girard & John Ogunsola & Georgia Perona-Wright & Dieudonné M Ngoyi & Nono Kuispond & Bruno Bucheton & Mamadou C, 2023. "IL-17 signalling is critical for controlling subcutaneous adipose tissue dynamics and parasite burden during chronic murine Trypanosoma brucei infection," Nature Communications, Nature, vol. 14(1), pages 1-21, December.
    • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42918-8
    DOI: 10.1038/s41467-023-42918-8
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    References listed on IDEAS

    as
    1. Salome A Bukachi & Simiyu Wandibba & Isaac K Nyamongo, 2017. "The socio-economic burden of human African trypanosomiasis and the coping strategies of households in the South Western Kenya foci," PLOS Neglected Tropical Diseases, Public Library of Science, vol. 11(10), pages 1-21, October.
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    4. Juan F. Quintana & Praveena Chandrasegaran & Matthew C. Sinton & Emma M. Briggs & Thomas D. Otto & Rhiannon Heslop & Calum Bentley-Abbot & Colin Loney & Luis de Lecea & Neil A. Mabbott & Annette MacLe, 2022. "Single cell and spatial transcriptomic analyses reveal microglia-plasma cell crosstalk in the brain during Trypanosoma brucei infection," Nature Communications, Nature, vol. 13(1), pages 1-19, December.
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