The XCL1/XCR1 axis is upregulated in type 1 diabetes and aggravates its pathogenesis
Camilla Tondello, … , Richard A. Kroczek, Urs Christen
Camilla Tondello, … , Richard A. Kroczek, Urs Christen
Published February 27, 2025
Citation Information: JCI Insight. 2025;10(7):e178743. https://doi.org/10.1172/jci.insight.178743.
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Research Article Immunology

The XCL1/XCR1 axis is upregulated in type 1 diabetes and aggravates its pathogenesis

Abstract

Type 1 diabetes (T1D) is precipitated by the autoimmune destruction of the insulin-producing β cells in the pancreatic islets of Langerhans. Chemokines have been identified as major conductors of islet infiltration by autoaggressive leukocytes, including antigen-presenting cells and islet autoantigen–specific T cells. We have previously generated a road map of gene expression in the islet microenvironment during T1D in a mouse model and found that most of the chemokine axes are chronically upregulated during T1D. The XCL1/XCR1 chemokine axis is of particular interest, since XCR1 is exclusively expressed on conventional DCs type 1 (cDC1) that excel by their high capacity for T cell activation. Here, we demonstrate that cDC1-expressing XCR1 are present in and around the islets of patients with T1D and of individuals with islet autoantibody positivity. Furthermore, we show that XCL1 plays an important role in the attraction of highly potent DCs expressing XCR1 to the islets in an inducible mouse model for T1D. XCL1-deficient mice display a diminished infiltration of XCR1+ cDC1 and, subsequently, a reduced magnitude and activity of islet autoantigen–specific T cells, resulting in a profound decrease in T1D incidence. Interference with the XCL1/XCR1 chemokine axis might constitute a novel therapy for T1D.

Authors

Camilla Tondello, Christine Bender, Gregory J. Golden, Deborah Puppe, Elisa Blickberndt, Monika Bayer, Giulia K. Buchmann, Josef Pfeilschifter, Malte Bachmann, Edith Hintermann, Ralf P. Brandes, Michael R. Betts, Richard A. Kroczek, Urs Christen

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Figure 6

XCL1-deficient mice show less T1D incidence.

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XCL1-deficient mice show less T1D incidence. (A) T1D incidence study com...
(A) T1D incidence study comparing RIP-GP and RIP-GP × XCL1–/– mice. Left panel: Percentage of diabetic mice at each time point after infection. Mice with nonfasting blood glucose (BG) levels of > 300 mg/dL were considered diabetic. Note that some mice reverted from a diabetic to a nondiabetic state over time. Right panel: Mean BG levels over time. Significant differences (2-way ANOVA) and the number of mice are indicated. (B) IHC staining of insulin in quick-frozen pancreas sections of RIP-GP and RIP-GP × XCL1–/– mice. Representative images are shown for days 7, 14, and 28 as well as week 12 after infection. Original magnification, 40×. Scale bars: 25 μm. Note that, for RIP-GP mice, it was not possible to acquire an image at week 12 (not done; n.d.), since all the mice had to be sacrificed earlier due to severe T1D. (C) Mean insulitis scores determined from insulin staining shown in B. Islets were scored as lined out in Methods. Insulitis in RIP-GP and RIP-GP × XCL1–/– mice was compared at days 7, 14, and 28 and at week 12 after infection. Number of mice are displayed in brackets.