Cells (Nov 2022)

Low-Dose rIL-15 Protects from Nephrotoxic Serum Nephritis via CD8<sup>+</sup> T Cells

  • Agnes A. Mooslechner,
  • Max Schuller,
  • Katharina Artinger,
  • Alexander H. Kirsch,
  • Corinna Schabhüttl,
  • Philipp Eller,
  • Alexander R. Rosenkranz,
  • Kathrin Eller

DOI
https://doi.org/10.3390/cells11223656
Journal volume & issue
Vol. 11, no. 22
p. 3656

Abstract

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Rapid progressive glomerulonephritis (GN) often leads to end-stage kidney disease, driving the need for renal replacement therapy and posing a global health burden. Low-dose cytokine-based immunotherapies provide a new strategy to treat GN. IL-15 is a strong candidate for the therapy of immune-mediated kidney disease since it has proven to be tubular-protective before. Therefore, we set out to test the potential of low-dose rIL-15 treatment in a mouse model of nephrotoxic serum nephritis (NTS), mimicking immune complex-driven GN in humans. A single low-dose treatment with rIL-15 ameliorated NTS, reflected by reduced albuminuria, less tissue scarring, fewer myeloid cells in the kidney, and improved tubular epithelial cell survival. In addition, CD8+ T cells, a primary target of IL-15, showed altered gene expression and function corresponding with less cytotoxicity mediated by rIL-15. With the use of transgenic knock-out mice, antibody depletion, and adoptive cell transfer studies, we here show that the beneficial effects of rIL-15 treatment in NTS depended on CD8+ T cells, suggesting a pivotal role for them in the underlying mechanism. Our findings add to existing evidence of the association of IL-15 with kidney health and imply a potential for low-dose rIL-15 immunotherapies in GN.

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