Iron supplementation alleviates pathologies in a mouse model of facioscapulohumeral muscular dystrophy
Kodai Nakamura, Huascar Pedro Ortuste Quiroga, Naoki Horii, Shin Fujimaki, Toshiro Moroishi, Keiichi I. Nakayama, Shinjiro Hino, Yoshihiko Saito, Ichizo Nishino, Yusuke Ono
Kodai Nakamura, Huascar Pedro Ortuste Quiroga, Naoki Horii, Shin Fujimaki, Toshiro Moroishi, Keiichi I. Nakayama, Shinjiro Hino, Yoshihiko Saito, Ichizo Nishino, Yusuke Ono
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Research Article Metabolism Muscle biology

Iron supplementation alleviates pathologies in a mouse model of facioscapulohumeral muscular dystrophy

Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is a genetic muscle disease caused by ectopic expression of the toxic protein DUX4, resulting in muscle weakness. However, the mechanism by which DUX4 exerts its toxicity remains unclear. In this study, we observed abnormal iron accumulation in muscles of patients with FSHD and in mice with muscle-specific DUX4 expression (DUX4-Tg mice). Treatment with iron chelators, an iron-deficient diet, and genetic modifications inhibiting intracellular uptake of iron did not improve but rather exacerbated FSHD pathology in DUX4-Tg mice. Unexpectedly, however, iron supplementation, from either a high-iron diet or intravenous iron administration, resulted in remarkable improvement in grip strength and running performance in DUX4-Tg mice. Iron supplementation suppressed abnormal iron accumulation and the ferroptosis-related pathway involving increased lipid peroxidation in DUX4-Tg muscle. Muscle-specific DUX4 expression led to retinal vasculopathy, a part of FSHD pathology, which was prevented by iron administration. Furthermore, high-throughput compound screening of the ferroptosis pathway identified drug candidates including ferrostatin-1 (Fer-1), a potent inhibitor of lipid peroxidation. Treatment with Fer-1 dramatically improved physical function in DUX4-Tg mice. Our findings demonstrate that DUX4-provoked toxicity is involved in the activation of the ferroptosis-related pathway and that supplementary iron could be a promising and readily available therapeutic option for FSHD.

Authors

Kodai Nakamura, Huascar Pedro Ortuste Quiroga, Naoki Horii, Shin Fujimaki, Toshiro Moroishi, Keiichi I. Nakayama, Shinjiro Hino, Yoshihiko Saito, Ichizo Nishino, Yusuke Ono

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Figure 8

Iron supplementation suppresses DUX4-activated ferroptosis-related pathway.

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Iron supplementation suppresses DUX4-activated ferroptosis-related pathw...
(A) Time course. Control or DUX4-Tg mice were fed ND or HID mixed with TMX at a concentration of 0.03 mg/g feed for 4 weeks as shown in Figure 4. (B and C) Immunoblot analysis for protein expression in quadriceps muscles (n = 8–11). (D) Immunohistochemistry for 8-OHdG and laminin to measure DNA damage in TA muscle (samples also used in Figure 5H). Scale bar: 100 μm; n = 7–11. (E) GSH/GSSG assay of biceps muscles (n = 5–7). (FI) Myoblasts were induced to differentiate into myotubes in culture as shown in Figure 1B. Cultured myotubes were treated with 20 μM DFO or 10 μM FAS for 48 hours in DM. Morphological analysis determined fusion index (H) and deformed myotube index (I). Arrowheads indicate deformed myotubes. Scale bar: 100 μm; n = 3–7. Data represent the mean ± SEM. P values were determined using 2-way or 1-way ANOVA followed by Tukey’s multiple-comparison post hoc test.