Interleukin-10 improves stroke outcome by controlling the detrimental Interleukin-17A response

Marius Piepke; Bettina H Clausen; Peter Ludewig; Jonas H Vienhues; Tanja Bedke; Ehsan Javidi; Björn Rissiek; Larissa Jank; Leonie Brockmann; Inga Sandrock; Karoline Degenhardt; Alina Jander; Vanessa Roth; Ines S Schädlich; Immo Prinz; Richard A Flavell; Yasushi Kobayashi; Thomas Renné; Christian Gerloff; Samuel Huber; Tim Magnus; Mathias Gelderblom

doi:10.1186/s12974-021-02316-7

Interleukin-10 improves stroke outcome by controlling the detrimental Interleukin-17A response

Marius Piepke
Bettina H Clausen
Peter Ludewig
Jonas H Vienhues
Tanja Bedke
Ehsan Javidi
Björn Rissiek
Larissa Jank
Leonie Brockmann
Inga Sandrock
Karoline Degenhardt
Alina Jander
Vanessa Roth
Ines S Schädlich
Immo Prinz
Richard A Flavell
Yasushi Kobayashi
Thomas Renné
Christian Gerloff
Samuel Huber
Tim Magnus
Mathias Gelderblom

Related Research units

Abstract

BACKGROUND: Lymphocytes have dichotomous functions in ischemic stroke. Regulatory T cells are protective, while IL-17A from innate lymphocytes promotes the infarct growth. With recent advances of T cell-subtype specific transgenic mouse models it now has become possible to study the complex interplay of T cell subpopulations in ischemic stroke.

METHODS: In a murine model of experimental stroke we analyzed the effects of IL-10 on the functional outcome for up to 14 days post-ischemia and defined the source of IL-10 in ischemic brains based on immunohistochemistry, flow cytometry, and bone-marrow chimeric mice. We used neutralizing IL-17A antibodies, intrathecal IL-10 injections, and transgenic mouse models which harbor a deletion of the IL-10R on distinct T cell subpopulations to further explore the interplay between IL-10 and IL-17A pathways in the ischemic brain.

RESULTS: We demonstrate that IL-10 deficient mice exhibit significantly increased infarct sizes on days 3 and 7 and enlarged brain atrophy and impaired neurological outcome on day 14 following tMCAO. In ischemic brains IL-10 producing immune cells included regulatory T cells, macrophages, and microglia. Neutralization of IL-17A following stroke reversed the worse outcome in IL-10 deficient mice and intracerebral treatment with recombinant IL-10 revealed that IL-10 controlled IL-17A positive lymphocytes in ischemic brains. Importantly, IL-10 acted differentially on αβ and γδ T cells. IL-17A producing CD4+ αβ T cells were directly controlled via their IL-10-receptor (IL-10R), whereas IL-10 by itself had no direct effect on the IL-17A production in γδ T cells. The control of the IL-17A production in γδ T cells depended on an intact IL10R signaling in regulatory T cells (Tregs).

CONCLUSIONS: Taken together, our data indicate a key function of IL-10 in restricting the detrimental IL-17A-signaling in stroke and further supports that IL-17A is a therapeutic opportunity for stroke treatment.

Bibliographical data

Original language	English
Article number	265
ISSN	1742-2094
DOIs	https://doi.org/10.1186/s12974-021-02316-7
Publication status	Published - 13.11.2021

Comment Deanary

PubMed	34772416