Tacrolimus- and sirolimus-induced human β cell dysfunction is reversible and preventable
Chunhua Dai, John T. Walker, Alena Shostak, Ana Padgett, Erick Spears, Scott Wisniewski, Greg Poffenberger, Radhika Aramandla, E. Danielle Dean, Nripesh Prasad, Shawn E. Levy, Dale L. Greiner, Leonard D. Shultz, Rita Bottino, Alvin C. Powers
Chunhua Dai, John T. Walker, Alena Shostak, Ana Padgett, Erick Spears, Scott Wisniewski, Greg Poffenberger, Radhika Aramandla, E. Danielle Dean, Nripesh Prasad, Shawn E. Levy, Dale L. Greiner, Leonard D. Shultz, Rita Bottino, Alvin C. Powers
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Research Article Endocrinology Metabolism

Tacrolimus- and sirolimus-induced human β cell dysfunction is reversible and preventable

Abstract

Posttransplantation diabetes mellitus (PTDM) is a common and significant complication related to immunosuppressive agents required to prevent organ or cell transplant rejection. To elucidate the effects of 2 commonly used agents, the calcineurin inhibitor tacrolimus (TAC) and the mTOR inhibitor sirolimus (SIR), on islet function and test whether these effects could be reversed or prevented, we investigated human islets transplanted into immunodeficient mice treated with TAC or SIR at clinically relevant levels. Both TAC and SIR impaired insulin secretion in fasted and/or stimulated conditions. Treatment with TAC or SIR increased amyloid deposition and islet macrophages, disrupted insulin granule formation, and induced broad transcriptional dysregulation related to peptide processing, ion/calcium flux, and the extracellular matrix; however, it did not affect regulation of β cell mass. Interestingly, these β cell abnormalities reversed after withdrawal of drug treatment. Furthermore, cotreatment with a GLP-1 receptor agonist completely prevented TAC-induced β cell dysfunction and partially prevented SIR-induced β cell dysfunction. These results highlight the importance of both calcineurin and mTOR signaling in normal human β cell function in vivo and suggest that modulation of these pathways may prevent or ameliorate PTDM.

Authors

Chunhua Dai, John T. Walker, Alena Shostak, Ana Padgett, Erick Spears, Scott Wisniewski, Greg Poffenberger, Radhika Aramandla, E. Danielle Dean, Nripesh Prasad, Shawn E. Levy, Dale L. Greiner, Leonard D. Shultz, Rita Bottino, Alvin C. Powers

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Figure 4

Ex-4 treatment can protect β cells from drug-induced dysfunction.

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Ex-4 treatment can protect β cells from drug-induced dysfunction. (A) Sc...
(A) Schematic of experimental design with TAC ± Ex-4 or SIR ± Ex-4 cotreatment for 4 weeks. (B and C) GTT and AUC treatment with TAC or SIR with or without Ex-4 for 4 weeks. (D–F) Blood glucose, human insulin, and human insulin/blood glucose ratios at 15 minutes after glucose-arginine stimulation (n = 7–10 samples/treatment from donors 4 and 5). (G and H) Representative images (G) of amyloid after 4 weeks of treatment and quantification (H; n = 3–4 grafts/treatment from 2 donors, donors 4 and 5 — see Supplemental Table 2 for raw data). Scale bar: 50 μm applies to all amyloid images. *P < 0.05. Data represent mean ± SEM. One-way ANOVA followed by Tukey multiple comparisons test was used for analysis of statistical significance. We highlight only the differences between TAC vs. TAC + Ex-4, or SIR vs. SIR + Ex-4 within panels C–F and H. Full statistical comparisons are shown in Supplemental Table 5.