Estrogen receptor–related receptor α regulation by interleukin‐1β in prostaglandin E₂– and cAMP‐dependent pathways in osteoarthritic chondrocytes

Abstract: Objective. We reported previously that the orphan nuclear receptor, estrogen receptor-related receptor ␣ (ERR␣), is expressed in articular chondrocytes and is dysregulated in a mouse model of inflammatory arthritis. The aim of this study, therefore, was to determine whether ERR␣ is also dysregulated in patients with osteoarthritis (OA).Methods. ERR␣ messenger RNA (mRNA) and protein were quantified in normal and OA cartilage samples and in OA chondrocytes in vitro, with and without short-term treatment with a v… Show more

“…1). Treatment with the ERRa inverse agonist XCT790, known to disrupt the interaction between ERRa and PGC1, decreased the expression of Sox9 in human OA chondrocytes, consistent with the view that ERRa and PGC1 together regulate Sox9 expression in chondrocytes supporting the hypothesis that they may function together in cartilage formation and maintenance (10) (Fig. 1).…”

“…(9,10) ERRa was also found to activate the Sox9 promoter and modulate Sox9 expression in a rat chondrogenic cell line (9) ( Fig. 1).…”

“…The data also implicate ERRa in cartilage maintenance in aging-related diseases such as rheumatoid arthritis and OA, where ERRa is dysregulated. (10,13) A role of ERRa in the Sox9 pathway is supported by the observation that one of its coactivators, PGC1a, is also expressed in chondrogenic sites where it coactivates Sox9 to regulate chondrogenesis (14) (Fig. 1).…”

“…1). Sox9 regulation by ERRa has been confirmed in patients with osteoarthritis (OA), a chronic disease characterized by slowly progressive destruction of the articular cartilage, (10,11) and in neonatal mouse calvarial explants overexpressing ERRa. (12) Experiments in which ERRa expression was downregulated in chondrogenic cells suggested that modulation of ERRa contributes to the maturation of proliferating chondrocytes to hypertrophy, most likely due to ERRa's direct or indirect regulation of Sox9.…”

“…In this article we do not review these in detail, but they include: (1) small heterodimer partner (SHP), which physically interacts with all three ERRs, repressing their activity (27)(28)(29) ; (2) hypoxia-inducible factor-a (HIF1a), which physically interacts with ERRa to stimulate HIF-induced transcription (30)(31)(32)(33) ; and (3) vascular endothelial growth factor (VEGF), which is a direct target gene of the ERRa/PGC1a complex and HIF1a in muscle and in breast cancer cells. (34,35) Several factors, including prostaglandin E1, BMP, and insulin-like growth factor 1, known to regulate ERRa or g expression and/or activity, also modulate VEGF production in bone cells, suggesting direct VEGF regulation by ERRa/g in OBs and OCs (10,25,38,39) ; (4) aryl hydrocarbon receptor (AhR), which has been reported to interact with ERa and ERRa (40)(41)(42)(43) ; (5) PPARa, which was reported to be directly regulated by ERRa in cardiac myocytes and skeletal muscles (44)(45)(46) ; and (6) Wnt11, which has been shown to be regulated in breast cancer cells by ERRa/b-catenin complex and in C3H10T1/2 cells through its interaction with PGC1a. (12,(47)(48)(49) Recently, we found osteoprotegerin (OPG) regulated in breast cancer cells impacting on bone metastases formation.…”

An energetic orphan in an endocrine tissue: A revised perspective of the function of estrogen receptor-related receptor alpha in bone and cartilage

“…1). Treatment with the ERRa inverse agonist XCT790, known to disrupt the interaction between ERRa and PGC1, decreased the expression of Sox9 in human OA chondrocytes, consistent with the view that ERRa and PGC1 together regulate Sox9 expression in chondrocytes supporting the hypothesis that they may function together in cartilage formation and maintenance (10) (Fig. 1).…”

“…(9,10) ERRa was also found to activate the Sox9 promoter and modulate Sox9 expression in a rat chondrogenic cell line (9) ( Fig. 1).…”

“…The data also implicate ERRa in cartilage maintenance in aging-related diseases such as rheumatoid arthritis and OA, where ERRa is dysregulated. (10,13) A role of ERRa in the Sox9 pathway is supported by the observation that one of its coactivators, PGC1a, is also expressed in chondrogenic sites where it coactivates Sox9 to regulate chondrogenesis (14) (Fig. 1).…”

“…1). Sox9 regulation by ERRa has been confirmed in patients with osteoarthritis (OA), a chronic disease characterized by slowly progressive destruction of the articular cartilage, (10,11) and in neonatal mouse calvarial explants overexpressing ERRa. (12) Experiments in which ERRa expression was downregulated in chondrogenic cells suggested that modulation of ERRa contributes to the maturation of proliferating chondrocytes to hypertrophy, most likely due to ERRa's direct or indirect regulation of Sox9.…”

“…In this article we do not review these in detail, but they include: (1) small heterodimer partner (SHP), which physically interacts with all three ERRs, repressing their activity (27)(28)(29) ; (2) hypoxia-inducible factor-a (HIF1a), which physically interacts with ERRa to stimulate HIF-induced transcription (30)(31)(32)(33) ; and (3) vascular endothelial growth factor (VEGF), which is a direct target gene of the ERRa/PGC1a complex and HIF1a in muscle and in breast cancer cells. (34,35) Several factors, including prostaglandin E1, BMP, and insulin-like growth factor 1, known to regulate ERRa or g expression and/or activity, also modulate VEGF production in bone cells, suggesting direct VEGF regulation by ERRa/g in OBs and OCs (10,25,38,39) ; (4) aryl hydrocarbon receptor (AhR), which has been reported to interact with ERa and ERRa (40)(41)(42)(43) ; (5) PPARa, which was reported to be directly regulated by ERRa in cardiac myocytes and skeletal muscles (44)(45)(46) ; and (6) Wnt11, which has been shown to be regulated in breast cancer cells by ERRa/b-catenin complex and in C3H10T1/2 cells through its interaction with PGC1a. (12,(47)(48)(49) Recently, we found osteoprotegerin (OPG) regulated in breast cancer cells impacting on bone metastases formation.…”

An energetic orphan in an endocrine tissue: A revised perspective of the function of estrogen receptor-related receptor alpha in bone and cartilage

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