Transient HIF2A inhibition promotes satellite cell proliferation and muscle regeneration
Liwei Xie, … , Jarrod A. Call, Hang Yin
Liwei Xie, … , Jarrod A. Call, Hang Yin
Published March 13, 2018
Citation Information: J Clin Invest. 2018;128(6):2339-2355. https://doi.org/10.1172/JCI96208.
View: Text | PDF
Research Article Muscle biology Article has an altmetric score of 32

Transient HIF2A inhibition promotes satellite cell proliferation and muscle regeneration

Abstract

The remarkable regeneration capability of skeletal muscle depends on the coordinated proliferation and differentiation of satellite cells (SCs). The self-renewal of SCs is critical for long-term maintenance of muscle regeneration potential. Hypoxia profoundly affects the proliferation, differentiation, and self-renewal of cultured myoblasts. However, the physiological relevance of hypoxia and hypoxia signaling in SCs in vivo remains largely unknown. Here, we demonstrate that SCs are in an intrinsic hypoxic state in vivo and express hypoxia-inducible factor 2A (HIF2A). HIF2A promotes the stemness and long-term homeostatic maintenance of SCs by maintaining their quiescence, increasing their self-renewal, and blocking their myogenic differentiation. HIF2A stabilization in SCs cultured under normoxia augments their engraftment potential in regenerative muscle. Conversely, HIF2A ablation leads to the depletion of SCs and their consequent regenerative failure in the long-term. In contrast, transient pharmacological inhibition of HIF2A accelerates muscle regeneration by increasing SC proliferation and differentiation. Mechanistically, HIF2A induces the quiescence and self-renewal of SCs by binding the promoter of the Spry1 gene and activating Spry1 expression. These findings suggest that HIF2A is a pivotal mediator of hypoxia signaling in SCs and may be therapeutically targeted to improve muscle regeneration.

Authors

Liwei Xie, Amelia Yin, Anna S. Nichenko, Aaron M. Beedle, Jarrod A. Call, Hang Yin

×

Figure 4

Long-term ablation of HIF2A results in the loss of SC homeostatic self-renewal.

Options: View larger image (or click on image) Download as PowerPoint
Long-term ablation of HIF2A results in the loss of SC homeostatic self-r...
(A) Timeline characterizing SC homeostasis after HIF2A ablation in QSCs. (B) Number of Pax7+ SCs per TA section in SC-HIF2AKO mice and control littermates on the same day of tamoxifen induction (+ Tamoxifen), 16 days, 1 month, and 6 months after tamoxifen-induced HIF2A ablation (n = 3 mice/group/time point). *P < 0.05 and ***P < 0.005, by 2-sided Student’s t test. Data represent the mean ± SEM. (C) H&E staining of TA muscles from SC-HIF2AKO mice and control littermates (n = 3 mice/group; 6 mo after tamoxifen-induced HIF2A ablation). Scar bars: 20 μm. (D) Distribution of myofiber cross-sectional areas of TA muscles from SC-HIF2AKO mice and control littermates (n = 3 mice/group; 6 mo after tamoxifen-induced HIF2A ablation).