Translational repression of HIF2α expression in mice with Chuvash polycythemia reverses polycythemia
Manik C. Ghosh, … , Michael A. Eckhaus, Tracey A. Rouault
Manik C. Ghosh, … , Michael A. Eckhaus, Tracey A. Rouault
Published February 26, 2018
Citation Information: J Clin Invest. 2018;128(4):1317-1325. https://doi.org/10.1172/JCI97684.
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Research Article Hematology

Translational repression of HIF2α expression in mice with Chuvash polycythemia reverses polycythemia

Abstract

Chuvash polycythemia is an inherited disease caused by a homozygous germline VHLR200W mutation, which leads to impaired degradation of HIF2α, elevated levels of serum erythropoietin, and erythrocytosis/polycythemia. This phenotype is recapitulated by a mouse model bearing a homozygous VhlR200W mutation. We previously showed that iron-regulatory protein 1–knockout (Irp1-knockout) mice developed erythrocytosis/polycythemia through translational derepression of Hif2α, suggesting that IRP1 could be a therapeutic target to treat Chuvash polycythemia. Here, we fed VhlR200W mice supplemented with Tempol, a small, stable nitroxide molecule and observed that Tempol decreased erythropoietin production, corrected splenomegaly, normalized hematocrit levels, and increased the lifespans of these mice. We attribute the reversal of erythrocytosis/polycythemia to translational repression of Hif2α expression by Tempol-mediated increases in the IRE-binding activity of Irp1, as reversal of polycythemia was abrogated in VhlR200W mice in which Irp1 was genetically ablated. Thus, a new approach to the treatment of patients with Chuvash polycythemia may include dietary supplementation of Tempol, which decreased Hif2α expression and markedly reduced life-threatening erythrocytosis/polycythemia in the VhlR200W mice.

Authors

Manik C. Ghosh, De-Liang Zhang, Hayden Ollivierre, Michael A. Eckhaus, Tracey A. Rouault

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Figure 2

Dietary Tempol supplementation prevented plethora, splenomegaly, and erythrocytosis/polycythemia in VhlR200W mice.

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Dietary Tempol supplementation prevented plethora, splenomegaly, and ery...
(A) The snouts and paws (indicated by white arrows) of VhlR200W mice appeared more reddish in color than did those of their WT littermates. The redness disappeared when the mutant mice were fed a Tempol-supplemented diet for 3 months. (B) Splenomegaly of VhlR200W mice was rescued by dietary Tempol supplementation, and the color of the spleens became lighter, suggesting that Tempol supplementation ameliorated the extramedullary erythropoiesis. (C and D) Hematocrit levels, as determined by capillary tube centrifugation, and (E) hemoglobin and (F) RBC levels of 5- to 8-month-old WT and VhlR200W mice fed a control or Tempol-supplemented diet showed that with the control diet, these parameters were elevated in VhlR200W mice, and Tempol supplementation significantly reduced hematocrit, hemoglobin, and RBC levels in the mutant mice. (DF) ***P < 0.001, by ordinary 1-way ANOVA (multiple comparisons).