4.7 Article

Nrf2/ARE Signaling Directly Regulates SOX9 to Potentially Alter Age-Dependent Cartilage Degeneration

ANTIOXIDANTS (2022)

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Journal

ANTIOXIDANTS
Volume 11, Issue 2, Pages -

Publisher

MDPI
DOI: 10.3390/antiox11020263

Keywords

SOX9; Nrf2; antioxidant response element; Keap1; osteoarthritis

Categories

Biochemistry & Molecular Biology Chemistry, Medicinal Food Science & Technology

Funding

  1. Excellence Initiative of the German Federal and State Governments
  2. Interdisciplinary Centre for Clinical Research of the Faculty of Medicine of the RWTH Aachen University [T9-3, T9-5, OC1-1]
  3. START Initiative [692057]
  4. Deutscher Akademischer Austauschdienst (DAAD) [57440921]
  5. Prosperos project - Interreg VA FlandersThe Netherlands program, CCI [2014TC16RFCB04]

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Oxidative stress is associated with osteoarthritis, and the Nrf2/ARE signaling pathway controls SOX9 expression. Nrf2 directly regulates SOX9 in articular cartilage, and the loss of Nrf2 may lead to mild osteoarthritis in old age.
Oxidative stress is implicated in osteoarthritis, and nuclear factor erythroid 2-related factor 2 (Nrf2)/antioxidant response element (ARE) pathway maintains redox homeostasis. We investigated whether Nrf2/ARE signaling controls SOX9. SOX9 expression in human C-28/I2 chondrocytes was measured by RT-qPCR after shRNA-mediated knockdown of Nrf2 or its antagonist the Kelch-like erythroid cell-derived protein with cap ''n'' collar homology-associated protein 1 (Keap1). To verify whether Nrf2 transcriptionally regulates SOX9, putative ARE-binding sites in the proximal SOX9 promoter region were inactivated, cloned into pGL3, and co-transfected with phRL-TK for dual-luciferase assays. SOX9 promoter activities without and with Nrf2-inducer methysticin were compared. Sox9 expression in articular chondrocytes was correlated to cartilage thickness and degeneration in wild-type (WT) and Nrf2-knockout mice. Nrf2-specific RNAi significantly decreased SOX9 expression, whereas Keap1-specific RNAi increased it. Putative ARE sites (ARE(1), ARE(2)) were identified in the SOX9 promoter region. ARE(2) mutagenesis significantly reduced SOX9 promoter activity, but ARE(1) excision did not. Functional ARE(2) site was essential for methysticin-mediated induction of SOX9 promoter activity. Young Nrf2-knockout mice revealed significantly lower Sox9-positive chondrocytes, and old Nrf2-knockout animals showed thinner cartilage and more cartilage degeneration. Our results suggest Nrf2 directly regulates SOX9 in articular cartilage, and Nrf2-loss can develop mild osteoarthritis at old age. Pharmacological Nrf2 induction may hold the potential to diminish age-dependent cartilage degeneration through improving SOX9 expression.

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