Immune checkpoint activity regulates polycystic kidney disease progression
Emily K. Kleczko, Dustin T. Nguyen, Kenneth H. Marsh, Colin D. Bauer, Amy S. Li, Marie-Louise T. Monaghan, Michael D. Berger, Seth B. Furgeson, Berenice Y. Gitomer, Michel B. Chonchol, Eric T. Clambey, Kurt A. Zimmerman, Raphael A. Nemenoff, Katharina Hopp
Emily K. Kleczko, Dustin T. Nguyen, Kenneth H. Marsh, Colin D. Bauer, Amy S. Li, Marie-Louise T. Monaghan, Michael D. Berger, Seth B. Furgeson, Berenice Y. Gitomer, Michel B. Chonchol, Eric T. Clambey, Kurt A. Zimmerman, Raphael A. Nemenoff, Katharina Hopp
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Research Article Nephrology

Immune checkpoint activity regulates polycystic kidney disease progression

Abstract

Innate and adaptive immune cells modulate the severity of autosomal dominant polycystic kidney disease (ADPKD), a common kidney disease with inadequate treatment options. ADPKD has parallels with cancer, in which immune checkpoint inhibitors have been shown to reactivate CD8+ T cells and slow tumor growth. We have previously shown that in PKD, CD8+ T cell loss worsens disease. This study used orthologous early-onset and adult-onset ADPKD models (Pkd1 p.R3277C) to evaluate the role of immune checkpoints in PKD. Flow cytometry of kidney cells showed increased levels of programmed cell death protein 1 (PD-1)/cytotoxic T lymphocyte associated protein 4 (CTLA-4) on T cells and programmed cell death ligand 1 (PD-L1)/CD80 on macrophages and epithelial cells in Pkd1RC/RC mice versus WT, paralleling disease severity. PD-L1/CD80 was also upregulated in ADPKD human cells and patient kidney tissue versus controls. Genetic PD-L1 loss or treatment with an anti–PD-1 antibody did not impact PKD severity in early-onset or adult-onset ADPKD models. However, treatment with anti–PD-1 plus anti–CTLA-4, blocking 2 immune checkpoints, improved PKD outcomes in adult-onset ADPKD mice; neither monotherapy altered PKD severity. Combination therapy resulted in increased kidney CD8+ T cell numbers/activation and decreased kidney regulatory T cell numbers correlative with PKD severity. Together, our data suggest that immune checkpoint activation is an important feature of and potential novel therapeutic target in ADPKD.

Authors

Emily K. Kleczko, Dustin T. Nguyen, Kenneth H. Marsh, Colin D. Bauer, Amy S. Li, Marie-Louise T. Monaghan, Michael D. Berger, Seth B. Furgeson, Berenice Y. Gitomer, Michel B. Chonchol, Eric T. Clambey, Kurt A. Zimmerman, Raphael A. Nemenoff, Katharina Hopp

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Figure 3

Genetic loss of Pd-l1 or monoclonal anti–PD-1 treatment does not affect PKD severity in mice with slowly or rapidly progressive ADPKD.

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Genetic loss of Pd-l1 or monoclonal anti–PD-1 treatment does not affect ...
(AD) Pkd1RC/RC mice were crossed with Pd-l1–/– (NCBI gene ID: Cd274) mice to obtain Pkd1RC/RC Cd274+/+ (control group; white) and Pkd1RC/RC Cd274–/– (experimental group; purple) mice. Animals were euthanized at 9 months of age in the C57BL/6J strain and 3 months in the BALB/cJ strain. (EH) 129S6/SvEvTac Pkd1RC/RC mice were treated with 10 mg/kg of anti–PD-1 (α-PD-1; blue) or IgG2a (control, white) twice weekly by i.p. injection from 4 to 6 months of age. (IL) C57BL/6J Pkd1RC/– mice were treated with 10 mg/kg of α-PD-1 (blue) or IgG2a (control, white) every other day by i.p. injection from P8 until P20. (A, E, and I) Representative H&E cross-sectional images of the kidneys. Scale bars: 1 mm. (B, F, and J) Percentage kidney weight/body weight (%KW/BW). (C, G, and K) Cystic index as measured by kidney area occupied by cysts (%). (D, H, and L) Blood urea nitrogen (BUN) levels. There was no significant difference in any of the analyzed PKD parameters, suggesting that inhibition of the PD-1|PD-L1 immune checkpoint does not impact adult-onset or early-onset PKD progression (also see Supplemental Table 3). Data are presented as mean ± SEM; single data points are depicted. Diamonds, males; circles, females. Red data points indicate the animal shown in A, E, and I. Nonparametric Mann-Whitney tests were performed. (AD) N = 10–14 for C57BL/6J or N = 6 for BALB/cJ mice per group. (EH) N = 15–16 mice per group. (IL) N = 6 mice per group.