Chondrocyte ferroptosis contribute to the progression of osteoarthritis

Yao, Xudong; Sun, Kai; Yu, Shengnan; Luo, Jun; Guo, Jiachao; Lin, Jheng-Hua; Wang, Genchun; Guo, Zhou; Ye, Yaping; Guo, Fengjing

doi:10.1016/j.jot.2020.09.006

Cited by 170 publications

(176 citation statements)

References 42 publications

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“…Our findings in vitro prompted us to further analyse the function of HIF‐2α downregulation in D‐mannose‐induced chondrocyte resistance to ferroptosis and OA progression in vivo. Consistent with previous studies which indicated the role of chondrocyte ferroptosis in OA progression, 9 , 10 immunofluorescence staining described above revealed a striking reduction of the key ferroptosis inhibitor, GPX4, in the articular chondrocytes upon ACLT surgery (Figure 3A ). To examine whether D‐mannose‐induced inhibition of HIF‐2α would protect osteoarthritic cartilage by suppressing chondrocyte ferroptosis, we fed mice with D‐mannose solution or water as previously described and then performed ACLT surgery.…”

Section: Resultssupporting

confidence: 92%

“…Recent evidence has indicated that chondrocyte ferroptosis contributes to chondrocyte homeostasis and osteoarthritic cartilage degeneration. 9 Similar to previous study, ferrostatin‐1 (Fer‐1), the inhibitor of ferroptosis, could attenuate the cytotoxicity of IL‐1β to chondrocytes, indicating the existence of ferroptosis in IL‐1β‐treated chondrocytes (Figure S2 A). GPX4 is a canonical glutathione‐based ferroptosis inhibitor and functions mainly through inhibiting the formation of lipid peroxides.…”

Section: Resultssupporting

confidence: 85%

“…Earlier research reported several ferroptosis‐related features, such as abnormal iron metabolism, 10 , 11 , 37 , 38 lipid peroxidation 39 , 40 and mitochondrial dysfunction, 41 , 42 are closely correlated with accelerating cartilage destruction. It is only recently that Yao et al 9 first demonstrated that chondrocyte ferroptosis contributes to the progression of osteoarthritis. In fact, besides ferroptosis, other forms of cell death, including necrosis, apoptosis and autophagy, of chondrocytes all interplay with cartilage degradation and OA progression.…”

Section: Discussionmentioning

confidence: 99%

“…Recent evidence has indicated that chondrocyte ferroptosis contributes to the progression of OA. 9 Iron‐overloaded mice exhibit increased cartilage destruction, and intracellular iron uptake is favoured in chondrocytes mimicking an OA phenotype. 10 , 11 These findings suggest that ferroptosis suppression is a novel candidate component for preventing OA progression.…”

Section: Introductionmentioning

confidence: 99%

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D‐mannose alleviates osteoarthritis progression by inhibiting chondrocyte ferroptosis in a HIF‐2α‐dependent manner

et al. 2021

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Section: Resultssupporting

confidence: 92%

Section: Resultssupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

D‐mannose alleviates osteoarthritis progression by inhibiting chondrocyte ferroptosis in a HIF‐2α‐dependent manner

et al. 2021

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“…In the present research, a highly selective inducer of iron overload, ferric ammonium citrate (FAC), was used to establish an iron overload model in porcine oocytes. FAC, a trivalent iron salt, is absorbed in vivo by reducing trivalent iron to divalent ferrous iron (Cotticelli et al, 2019;Yao et al, 2021). It has been shown that FAC-induced intracellular iron overload causes ferroptosis (Fang et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

Iron Overload-Induced Ferroptosis Impairs Porcine Oocyte Maturation and Subsequent Embryonic Developmental Competence in vitro

Zhang

Wang

et al. 2021

Front. Cell Dev. Biol.

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Accumulating evidence indicates that ferroptosis is an iron-dependent form of regulated cell death. This type of iron-dependent programmed cell death is different from traditional forms of regulated cell death, such as apoptosis and autophagy. However, the role of ferroptosis in porcine oocyte maturation and the associated mechanism remain unclear. In the present research, we investigated the effects of ferric ammonium citrate (FAC), a specific ferroptosis inducer, on porcine oocyte meiotic maturation and quality and subsequent embryonic developmental competence. FAC treatment caused obvious accumulation of intracellular ferrous ions in porcine oocytes. At the end of the in vitro maturation (IVM) period, there was a significant decrease in the polar body (PB) extrusion rate and an increase in the percentage of abnormal oocytes in the FAC treatment groups, indicating that iron overload-induced ferroptosis may suppress the meiotic process during porcine oocyte maturation. We also found that after FAC treatment, the subsequent two-cell rate, four-cell rate and blastocyst formation rate were significantly decreased in porcine parthenogenetic activation (PA) embryos, indicating that iron overload-induced ferroptosis decreased porcine oocyte quality. Further analysis revealed that FAC treatment not only enhanced intracellular reactive oxygen species (ROS) generation, decreased intracellular free thiol levels and induced mitochondrial dysfunction but also triggered autophagy in porcine oocytes. Taken together, these findings suggest that iron overload-induced ferroptosis impairs porcine oocyte meiosis and decreases porcine oocyte quality, possibly by increasing oxidative stress, inducing mitochondrial dysfunction and triggering autophagy.

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Targeting Endogenous Hydrogen Peroxide at Bone Defects Promotes Bone Repair

Han

et al. 2021

Adv Funct Materials

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Reactive oxygen species (ROS) plays a critical role in tissue repair, including bone. Therefore, detecting and regulating ROS is essential for monitoring and facilitating bone repair. In this study, for the first time, the spatiotemporal profile of ROS, represented by hydrogen peroxide (H2O2), in the bone injury microenvironment using photoacoustic imaging technique is visualized. The ROS levels significantly increase upon bone injury, peak at a certain stage of bone healing, and then gradually decrease toward baseline level. To regulate ROS in the bone injury microenvironment, the use of hollow manganese dioxide nanoparticles (hMNPs), which are able to decompose H2O2 and generate oxygen is explored. In vitro, hMNPs eliminate intracellular ROS to protect cells from oxidative damage and facilitate cell growth by releasing oxygen. In vivo, composite hydrogels containing gelatin methacryloyl (GelMA) and hMNPs (hMNP/GelMA) release oxygen and bone morphogenetic protein‐2 (BMP‐2)‐associated peptide in an “on‐demand” fashion in response to bone microenvironmental ROS change. Applying hMNP/GelMA composite hydrogels loaded with BMP‐2‐associated peptide (BhMNP/GelMA) significantly enhances bone formation in a rat critical‐sized calvarial defect. Together, findings from this study imply that the visualization and regulation of ROS such as H2O2 may be a novel strategy for diagnosing and treating bone defects.

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Chondrocyte ferroptosis contribute to the progression of osteoarthritis

Cited by 170 publications

References 42 publications

D‐mannose alleviates osteoarthritis progression by inhibiting chondrocyte ferroptosis in a HIF‐2α‐dependent manner

D‐mannose alleviates osteoarthritis progression by inhibiting chondrocyte ferroptosis in a HIF‐2α‐dependent manner

Iron Overload-Induced Ferroptosis Impairs Porcine Oocyte Maturation and Subsequent Embryonic Developmental Competence in vitro

Targeting Endogenous Hydrogen Peroxide at Bone Defects Promotes Bone Repair

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