What question did this study set out to answer?

The aim is to explore the molecular mechanisms by which DMOG pretreatment affects osteogenic and adipogenic balance in ONFH-derived BMSCs.

April 21, 2026Open Access

DMOG pretreatment restores osteogenic–adipogenic balance and mitochondrial function in ONFH BMSCs through the HIF-1α/Homer3 pathway

Key Points

The aim is to explore the molecular mechanisms by which DMOG pretreatment affects osteogenic and adipogenic balance in ONFH-derived BMSCs.
Isolated BMSCs from ONFH patients' femoral heads and iliac crests.
Performed functional assays, RNA sequencing, and molecular analyses.
Conducted loss-of-function experiments targeting HIF-1α and Homer3.
fhBMSCs showed impaired osteogenesis and enhanced adipogenesis compared to iBMSCs.
DMOG pretreatment improved osteogenic differentiation and mitochondrial dynamics.
Homer3 was identified as a negative regulator of HIF-1α and its knockdown mimicked DMOG effects.

Abstract

Osteonecrosis of the femoral head (ONFH) is a progressive orthopedic disorder that often culminates in femoral head collapse and joint failure. Dysfunction of bone marrow mesenchymal stem cells (BMSCs), including impaired osteogenesis, enhanced adipogenesis, and mitochondrial dysfunction, has been increasingly recognized as a central driver of ONFH pathogenesis. However, the molecular mechanisms linking metabolic stress to lineage imbalance remain poorly defined. Paired BMSCs were isolated from necrotic femoral head regions (fhBMSCs) and the iliac crest (iBMSCs) of ONFH patients. Functional assays, RNA sequencing, and molecular analyses were performed to evaluate the effects of the hypoxia mimetic dimethyloxalylglycine (DMOG) on osteogenic–adipogenic balance, mitochondrial function, and senescence. Loss-of-function experiments targeting hypoxia-inducible factor-1α (HIF-1α) and Homer3 were conducted to elucidate mechanistic pathways. Compared with iBMSCs, fhBMSCs exhibited impaired osteogenesis, enhanced adipogenesis, mitochondrial dysfunction, and increased senescence. DMOG pretreatment restored osteogenic differentiation, suppressed adipogenesis, improved mitochondrial dynamics, reduced oxidative stress, and enhanced bioenergetic metabolism. These protective effects were dependent on HIF-1α stabilization. Transcriptomic profiling identified Homer3 as a downstream negative regulator of HIF-1α. Homer3 was aberrantly upregulated in fhBMSCs but suppressed by DMOG, and its knockdown mimicked the effects of DMOG by promoting osteogenesis, inhibiting adipogenesis, enhancing mitophagy, and restoring mitochondrial function. Conversely, silencing HIF-1α abolished DMOG-mediated benefits and reinstated Homer3 expression. This study identifies the HIF-1α/Homer3 axis as a central regulator of lineage balance and mitochondrial homeostasis in ONFH-derived BMSCs. Pharmacological targeting of this pathway with DMOG or related prolyl hydroxylase inhibitors may provide a promising joint-preserving therapeutic strategy for ONFH.

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Cite This Study

Chen et al. (Sun,) studied this question.

synapsesocial.com/papers/69e7143fcb99343efc98d972 https://doi.org/https://doi.org/10.1186/s13287-026-05026-0

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