| Literature DB >> 26851078 |
Jia-Jie Hu1,2, Zi Yin1,2, Wei-Liang Shen3, Yu-Bin Xie1,2, Ting Zhu1,2, Ping Lu1,2, You-Zhi Cai4, Min-Jian Kong3, Boon Chin Heng5, Yi-Ting Zhou1,6, Wei-Shan Chen3, Xiao Chen1,2, Hong-Wei Ouyang1,2,7,8,9.
Abstract
Calcification of soft tissues, such as heart valves and tendons, is a common clinical problem with limited therapeutics. Tissue specific stem/progenitor cells proliferate to repopulate injured tissues. But some of them become divergent to the direction of ossification in the local pathological microenvironment, thereby representing a cellular target for pharmacological approach. We observed that HIF-2alpha (encoded by EPAS1 inclined form) signaling is markedly activated within stem/progenitor cells recruited at calcified sites of diseased human tendons and heart valves. Proinflammatory microenvironment, rather than hypoxia, is correlated with HIF-2alpha activation and promoted osteochondrogenic differentiation of tendon stem/progenitor cells (TSPCs). Abnormal upregulation of HIF-2alpha served as a key switch to direct TSPCs differentiation into osteochondral-lineage rather than teno-lineage. Notably, Scleraxis (Scx), an essential tendon specific transcription factor, was suppressed on constitutive activation of HIF-2alpha and mediated the effect of HIF-2alpha on TSPCs fate decision. Moreover, pharmacological inhibition of HIF-2alpha with digoxin, which is a widely utilized drug, can efficiently inhibit calcification and enhance tenogenesis in vitro and in the Achilles's tendinopathy model. Taken together, these findings reveal the significant role of the tissue stem/progenitor cells fate decision and suggest that pharmacological regulation of HIF-2alpha function is a promising approach for soft tissue calcification treatment.Entities:
Keywords: Calcification; Digoxin; HIF-2 alpha; Heart valves; Stem cells; Tendons
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Year: 2016 PMID: 26851078 DOI: 10.1002/stem.2306
Source DB: PubMed Journal: Stem Cells ISSN: 1066-5099 Impact factor: 6.277