Your search keyword '"Zhao, Hongyan"' showing total 9 results

1. Antiosteoclastic bone resorption activity of osteoprotegerin via enhanced AKT/mTOR/ULK1‐mediated autophagic pathway.

Author

Zhao, Hongyan, Sun, Ziqiang, Ma, Yonggang, Song, Ruilong, Yuan, Yan, Bian, Jianchun, Gu, Jianhong, and Liu, Zongping

Subjects

*BONE resorption, *PROTEIN kinase B, *MACROPHAGE colony-stimulating factor, *OSTEOCLAST inhibition

Abstract

Autophagy plays a critical role in the maintenance of bone homeostasis. Osteoprotegerin (OPG) is an inhibitor of osteoclast‐mediated bone resorption. However, whether autophagy is involved in the antiosteoclastogenic effects of OPG remains unclear. The present study aimed to investigate the potential mechanism of autophagy during OPG‐induced bone resorption via inhibition of osteoclasts differentiated from bone marrow‐derived macrophages in BALB/c mice. The results showed that after treatment with receptor activator of nuclear factor‐κΒ ligand and macrophage colony‐stimulating factor for 3 days, TRAP+ osteoclasts formed, representing the resting state of autophagy. These osteoclasts were treated with OPG and underwent autophagy, as demonstrated by LC3‐II accumulation, acidic vesicular organelle formation, and the presence of autophagosomes. The levels of autophagy‐related proteins, LC3‐II increased and P62 decreased at 3 hr in OPG‐treated osteoclasts. The viability, differentiation, and bone resorption activity of osteoclasts declined after OPG treatment. Treatment with OPG and chloroquine, an autophagy inhibitor, attenuated OPG‐induced inhibition of osteoclastic bone resorption, whereas rapamycin (RAP), an autophagy inducer, enhanced OPG‐induced inhibition of differentiation, survival, and bone resorption activity of osteoclasts. Furthermore, OPG reduced the amount of phosphorylated(p) protein kinase B (AKT) and pmTOR and increased the level of pULK, in a dose‐dependant manner. LY294002, a phosphatidylinositol‐4,5‐bisphosphate 3‐kinase (PI3K)/AKT pathway inhibitor, attenuated the decline in pAKT, but enhanced the decline in pmTOR and the increase in pULK1 following OPG treatment. RAP enhanced the OPG‐induced increase in pULK1. The PI3K inhibitor 3‐methyladenine partly blocked OPG‐induced autophagy. Thus, the results revealed that OPG inhibits osteoclast bone resorption by inducing autophagy via the AKT/mTOR/ULK1 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2020

2. Boldine isolated from Litsea cubeba inhibits bone resorption by suppressing the osteoclast differentiation in collagen-induced arthritis.

Author

Zhao, Hongyan, Xu, Huihui, Qiao, Senyan, Lu, Cheng, Wang, Gui, Liu, Meijie, Guo, Baosheng, Tan, Yong, Ju, Dahong, and Xiao, Cheng

Subjects

*ARTHRITIS, *BONE resorption, *OSTEOCLASTS, *CELL differentiation, *MOLECULAR pharmacology

Abstract

Objective To investigate the effect of boldine isolated from Litsea cubeba on collagen-induced arthritis (CIA) rats and explore the molecular mechanism predicted by network pharmacology. Material and methods CIA rats were orally administered with boldine. The bone destruction of paws was analyzed by histologic examination, tartrate-resistant acid phosphatase (TRACP) staining and micro-computed tomography. Prediction of signal pathway associated with boldine network molecules and CIA genes was applied by the network pharmacology analysis. The expressions of osteoprotegerin (OPG), receptor activator of nuclear factor-κB (RANK) and its ligand (RANKL) in the ankle were detected by immunohistochemistry. In vitro osteoclasts were cultured in the presence of variable doses of boldine and the RANK expressions were evaluated using Real-time polymerase chain reaction and western blot. Results Boldine reduced ankle swelling, alleviated pathological damage and significantly prevented bone destruction in CIA rats. Consistent with this, enzyme linked immunosorbent assay revealed boldine decreased serum TRACP5b levels and osteoclast number in the ankle region by TRACP staining from CIA rats. The network pharmacology analysis indicated that RANK signaling in osteoclasts was the most significant canonical pathway associated with boldine network molecules and CIA genes, which was verified by the increased expression of OPG, reduced expression of RANK, RANKL and RANKL/OPG in boldine-treated CIA rats. The in vitro study further confirmed that boldine inhibited osteoclastogenesis by inhibiting the RANKL/RANK signaling pathway. Conclusion Taken together, our study first indicates that boldine from Litsea cubeba suppresses osteoclastogenesis, improves bone destruction by down-regulating the OPG/RANKL/RANK signal pathway and may be a potential therapeutic agent for rheumatoid arthritis. [ABSTRACT FROM AUTHOR]

Published

2017

3. Osteoprotegerin induces podosome disassembly in osteoclasts through calcium, ERK, and p38 MAPK signaling pathways.

Author

Zhao, Hongyan, Liu, Xuezhong, Zou, Hui, Dai, Nannan, Yao, Lulian, Gao, Qian, Liu, Wei, Gu, Jianhong, Yuan, Yan, Bian, Jianchun, and Liu, Zongping

Subjects

*OSTEOPROTEGERIN, *OSTEOCLASTS, *MITOGEN-activated protein kinases, *EXTRACELLULAR signal-regulated kinases, *CELLULAR signal transduction, *INTRACELLULAR calcium

Abstract

Osteoclasts are critical for bone resorption and use podosomes to attach to bone matrix. Osteoprotegerin (OPG) is a negative regulator of osteoclast function that can affect the formation and function of podosomes. However, the signaling pathways that link OPG to podosome function have not been well characterized. Therefore, this study examined the roles of intracellular calcium and MAPKs in OPG-induced podosome disassembly in osteoclasts. We assessed the effects of the intracellular calcium chelator Bapta-AM, ERK inhibitor U0126, and p38 inhibitor SB202190 on OPG-treated osteoclast differentiation, adhesion structures, intracellular free Ca 2+ concentration and the phosphorylation state of podosome associated proteins (Pyk2 and Src). Mouse monocytic RAW 264.7 cells were differentiated to osteoclasts using RANKL (30 ng/mL) and M-CSF (25 ng/mL). The cells were pretreated with Bapta-AM (5 μM), U0126 (5 μM), or SB202190 (10 μM) for 30 min, followed by 40 ng/mL OPG for 3 h. Osteoclastogenesis, adhesion structure, viability and morphology, intracellular free Ca 2+ concentration and the phosphorylation state of Pyk2 and Src were measured by TRAP staining, scanning electron microscopy, real-time cell analyzer, flow cytometry and western blotting, respectively. OPG significantly inhibited osteoclastogenesis, the formation of adhesion structures, and reduced the amount of phosphorylated Pyk2 and Src-pY527, but increased phosphorylation of Src-pY416. Bapta-AM, U0126, and SB202190 partially restored osteoclast differentiation and adhesion structures. Both Bapta-AM and U0126, but not SB202190, restored the levels of intracellular free Ca 2+ concentration, phosphorylated Pyk2 and Src-pY527. All three inhibitors blocked OPG-induced phosphorylation at Src-pY416. These results suggest OPG disrupts the attachment structures of osteoclasts and activates Src as an adaptor protein that competes for the reduced amount of phosphorylated Pyk2 through calcium- and ERK-dependent signaling pathways. p38 MAPK signaling may have a different role in OPG-induced osteoclast retraction. Our findings potentially offer novel insights into the signaling mechanisms downstream of OPG that affect osteoclast attachment to the extracellular matrix. [ABSTRACT FROM AUTHOR]

Published

2015

4. The effect of P2X7R-mediated Ca2+ signaling in OPG-induced osteoclasts adhesive structure damage.

Author

Ma, Yonggang, Zhao, Hongyan, Chile, Chung, Wang, Chao, Zheng, Jiaming, Song, Ruilong, Zou, Hui, Gu, Jianhong, YanYuan, Bian, Jianchun, and Liu, Zongping

Subjects

*OSTEOCLASTOGENESIS, *PROTEIN-tyrosine kinases, *PURINERGIC receptors, *BONE resorption, *TRANSCRIPTION factors, *OSTEOPROTEGERIN, *DESMOGLEINS, *CD54 antigen

Abstract

Osteoclast adhesion is important for bone resorption. Osteoprotegerin inhibits osteoclast differentiation and bone resorption via Ca2+ signaling. Purinergic receptor P2X7 (P2X7R) affects osteoclastogenesis by activating transcription factor nuclear factor of activated T cells 1 (NFATc1). However, the detailed mechanism of osteoprotegerin-mediated P2X7R modulation of osteoclast adhesion is unclear. This study aimed to determine the effect of P2X7R on osteoprotegerin-induced damage to osteoclast adhesion. Osteoprotegerin reduced the expression of P2X7R, and protein tyrosine kinase 2 (PYK2) and SRC phosphorylation, and reduced calcium concentration, significantly decreasing Ca2+-NFATc1 signaling. 1,2-Bis(2-aminophenoxy)ethane-N,N,N′,N'-tetraacetic acid tetrakis (acetoxymethyl ester) (BAPTA-AM)/ N -(6-Aminohexyl)-5-chloro-1-naphthalenesulfonamide hydrochloride (W-7) partly or absolutely recovered osteoprotegerin-induced osteoclasts adhesion structure damage, including increased the PYK2 and SRC phosphorylation, changed the distribution of PYK2/SRC and integrinαvβ3, and inhibited retraction of lamellipodia and filopodia and recovered osteoclast bone resorption activity. In addition, BAPTA-AM/W-7 also increased osteoprotegerin-induced activation of Ca2+-NFATc1 signaling, and restored normal P2X7R levels. P2X7R knockdown significantly inhibited osteoclast differentiation, and the formation of lamellipodia and filopodia, reduced the PYK2 and SRC phosphorylation, and inhibited Ca2+-related protein activation. However, P2X7R knockdown aggravated osteoprotegerin-induced osteoclast adhesion damage via Ca2+ signaling. In conclusion, the P2X7R–Ca2+ NFATc1 signaling pathway has a key functional role in osteoprotegerin-induced osteoclast adhesion structure damage. [ABSTRACT FROM AUTHOR]

Published

2019

5. The Mechanism of Osteoprotegerin-Induced Osteoclast Pyroptosis In Vitro.

Author

Zhu, Jiaqiao, Ma, Yonggang, Wang, Jie, Wang, Yangyang, Ali, Waseem, Zou, Hui, Zhao, Hongyan, Tong, Xishuai, Song, Ruilong, and Liu, Zongping

Subjects

*OSTEOCLASTOGENESIS, *PYROPTOSIS, *NF-kappa B, *TUMOR necrosis factors, *CELL death, *CELL membranes

Abstract

Osteoprotegerin (OPG) is a new member of the tumor necrosis factor (TNF) receptor superfamily, which can inhibit the differentiation and activity of osteoclasts by binding to nuclear factor kappa B receptor activator (RANK) competitively with nuclear factor kappa B receptor activator ligand (RANKL). The previous experiments found that OPG can induce apoptosis of mature osteoclasts in vitro, which can inhibit the activity of mature osteoclasts, thereby exerting its role in protecting bone tissue. In addition, pyroptosis is a new type of cell death that is different from apoptosis. It is unclear whether OPG can induce mature osteoclast pyroptosis and thereby play its role in protecting bone tissue. In this study, the results showed that compared with the control group, the survival rate of osteoclasts in the OPG group was significantly reduced, and the contents of IL-1β, IL-18, and LDH in the supernatant both increased. Many osteoclast plasma membranes were observed to rupture in bright fields, and OPG induced loss of their morphology. Flow cytometry was used to analyze the pyroptosis rate; OPG significantly increased the osteoclast pyroptosis rate. To further reveal the mechanism of OPG-induced osteoclast pyroptosis, we examined the expression level of pyroptosis-related genes and proteins, and the results found that OPG increased the expression of NLRP3, ASC, caspase-1, and GSDMD-N compared with the control group. In summary, OPG can induce osteoclast pyroptosis, and its mechanism is related to the expression levels of ASC, NLRP3, caspase 1 and GSDMD, which were included in the classical pathway of pyroptosis. [ABSTRACT FROM AUTHOR]

Published

2023

6. P2X7 receptor knockdown suppresses osteoclast differentiation by inhibiting autophagy and Ca2+/calcineurin signaling.

Author

Ma, Yonggang, Di, Ran, Zhao, Hongyan, Song, Ruilong, Zou, Hui, and Liu, Zongping

Subjects

*OSTEOCLASTS, *OSTEOCLASTOGENESIS, *AUTOPHAGY, *ACID phosphatase, *BONE diseases, *PROTEIN expression, *T cells

Abstract

Bone is continuously remodeled in a dynamic process maintained by osteoclasts and osteoblasts, and imbalances in the relative activities of these cell types can cause various pathological conditions, including rheumatoid arthritis and osteoporosis. Osteoclasts are multinucleated cells that serve an important role in regulating the development of osteoporosis. Furthermore, P2X7 receptor activation has a vital role in physiological and pathological reactions in bone, including bone disease. Therefore, the present study aimed to investigate the effect of P2X7 receptor on osteoclast differentiation and to explore the underlying molecular mechanism by western blotting and tartrate-resistant acid phosphatase staining. The results indicated that the expression levels of P2X7 receptor and intracellular Ca2+ concentration levels were very high in mature osteoclasts. Furthermore, P2X7 receptor overexpression increased the number of multinucleated osteoclasts and the expression of osteoclastogenesis-related proteins. P2X7 receptor overexpression was also associated with downstream activation of Ca2+/calcineurin/nuclear factor of activated T cells c1 (NFATc1) signaling and increased expression of autophagy-related proteins during osteoclast differentiation. By contrast, knockdown of P2X7 receptor exerted the opposite effects. Notably, FK506 (a Ca2+/calcineurin/NFATc1 signaling inhibitor) abrogated P2X7 receptor overexpression-induced osteoclast differentiation and activation of autophagy. Moreover, 3-MA (an autophagy inhibitor) significantly suppressed P2X7 receptor overexpression-induced osteoclast differentiation. In conclusion, P2X7 receptor knockdown may suppress osteoclast differentiation by modulating autophagy and the Ca2+/calcineurin/NFATc1 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2022

7. Cadmium toxicity: A role in bone cell function and teeth development.

Author

Ma, Yonggang, Ran, Di, Shi, Xueni, Zhao, Hongyan, and Liu, Zongping

Abstract

Cadmium (Cd) is a widespread environmental contaminant that causes severe bone metabolism disease, such as osteoporosis, osteoarthritis, and osteomalacia. The present review aimed to explore the molecular mechanisms of Cd-induced bone injury starting from bone cell function and teeth development. Cd inhibits the differentiation of bone marrow mesenchymal stem cells (BMSCs) into osteoblasts, and directly causes BMSC apoptosis. In the case of osteoporosis, Cd mainly affects the activation of osteoclasts and promotes bone resorption. Cd-induces osteoblast injury and oxidative stress, which causes DNA damage, mitochondrial dysfunction, and endoplasmic reticulum stress, resulting in apoptosis. In addition, the development of osteoarthritis (OA) might be related to Cd-induced chondrocyte damage. The high expression of metallothionein (MT) might reduce Cd toxicity toward osteocytes. The toxicity of Cd toward teeth mainly focuses on enamel development and dental caries. Understanding the effect of Cd on bone cell function and teeth development could contribute to revealing the mechanisms of Cd-induced bone damage. This review explores Cd-induced bone disease from cellular and molecular levels, and provides new directions for removing this heavy metal from the environment. Cd exposure causes severe bone metabolism disease. Apoptosis and differentiation play an essential role in Cd-induced osteoporosis. The development of osteoarthritis (OA) might be related to Cd-induced chondrocyte damage. The expression of MT may affect Cd-induced osteocytes damage. The toxicity of Cd toward teeth is mainly focused on enamel development and dental caries. Therefore, bone cells function and teeth development is mainly present manner of Cd toxicity. Unlabelled Image • Cd causes severe bone metabolism disease. • Cd-induces bone injury via affecting bone cell formation and function. • Apoptosis is main death manner by Cd-induced bone cell. • The toxicity of Cd toward teeth is mainly affected enamel development and dental caries. [ABSTRACT FROM AUTHOR]

Published

2021

8. The effect of P2X7 on cadmium-induced osteoporosis in mice.

Author

Ma, Yonggang, Ran, Di, Cao, Ying, Zhao, Hongyan, Song, Ruilong, Zou, Hui, Gu, Jianhong, Yuan, Yan, Bian, Jianchun, Zhu, Jiaqiao, and Liu, Zongping

Subjects

*CADMIUM poisoning, *OSTEOBLASTS, *BONE marrow cells, *OSTEOPOROSIS, *BONE cells, *POLLUTANTS, *BONE marrow

Abstract

Cadmium (Cd), an environmental pollutant, induces osteoporosis by directly destroying bone tissue, but its direct damaging effect on bone cells is not fully illustrated. Here, we treated mouse bone marrow stem cells (BMSC) and bone marrow macrophages (BMM) with Cd, and gave BALB/c mice Cd in water. Long-term Cd exposure significantly inhibited BMSC osteogenesis and osteoclast differentiation in vitro , and induced osteoporosis in vivo. Cd exposure also reduced P2X7 expression dramatically. However, P2X7 deletion significantly inhibited osteoblast and osteoclast differentiation; P2X7 overexpression obviously reduced the suppression effect of Cd on osteoblast and osteoclast differentiation. The suppression of P2X7–PI3K–AKT signaling aggravated the effect of Cd. In mice, short-term Cd exposure did not result in osteoporosis, but bone formation was inhibited, RANKL expression was increased, and osteoclasts were significantly increased in vivo. In vitro , short-term Cd exposure not only increased osteoclast numbers, but also promoted osteoclast adhesion function at late-stage osteoclast differentiation. Cd exposure also reduced P2X7 expression in vivo and in vitro. Our results demonstrate that short-term Cd exposure does not affect osteoblast and osteoclast apoptosis in vivo and in vitro , but long-term Cd exposure significantly increases bone tissue apoptosis. Overall, our results describe a novel mechanism for Cd-induced osteoporosis. ga1 • Long-term Cd exposure induced osteoporosis in mice. • Cd exposure decreased P2X7 greatly in vitro and in vivo. • In vitro , deleting P2X7 inhibited osteoblast and osteoclast differentiation. • Cd exposure inhibited osteogenesis and osteoclast differentiation in vitro. • P2X7 overexpression decreased this suppressive effect of Cd. [ABSTRACT FROM AUTHOR]

Published

2021

9. Ca2+/CaM/CaMK signaling is involved in cadmium-induced osteoclast differentiation.

Author

Liu, Wei, Le, Chung Chi, Wang, Dong, Ran, Di, Wang, Yi, Zhao, Hongyan, Gu, Jianhong, Zou, Hui, Yuan, Yan, Bian, Jianchun, and Liu, Zongping

Subjects

*INTRACELLULAR calcium, *BONE resorption, *OSTEOCLASTS, *BONE density, *MACROPHAGE colony-stimulating factor, *CALCIUM ions, *TRANCE protein, *BONE marrow

Abstract

Schematic representation of the proposed Cd-induced signaling pathway in osteoclasts. Treatment of osteoclasts with Cd leads to a transient increase in intracellular calcium concentration ([Ca2+] i). Cd-induces the elevation of [Ca2+] i and activation of CaM/CaMKII/CaMKIV signaling. CaM/CaMKII/CaMKIV signaling induces the expression of NFATc1, leading to osteoclast differentiation. ER Ca2+ release, the elevation of [Ca2+] I , and the activation of CaM, CaMKII, and CaMKIV can be inhibited by 2-APB, BAPTA-AM, W-7, KN93 and STO-609, respectively. Environmental cadmium (Cd) pollution can ultimately lead to chronic toxicity via food consumption. Previous studies have demonstrated that long-term low-dose Cd exposure decreases bone mineral density and bone mineralization. Cd may increase receptor activator of nuclear factor-κ B ligand (RANKL) expression by osteoclasts, and inhibit the expression of osteoprotegerin. However, the molecular mechanism underlying Cd toxicity toward osteoclasts is unclear. In this study, bone marrow monocytes were isolated from C57BL/6 mice and treated with macrophage colony-stimulating factor and RANKL to induce the formation of osteoclasts. The results show that low-dose Cd exposure induced osteoclast differentiation. Cd also increased the intracellular calcium concentration of osteoclasts by triggering release of calcium ions from the endoplasmic reticulum into the cytoplasm. Furthermore, the elevation of intracellular calcium levels was shown to activate the calmodulin (CaM)/calmodulin-dependent protein kinase (CaMK) pathway. NFATc1 is a downstream protein of CaM/CaMK signaling, as well as a key player in osteoclast differentiation. Overall, we conclude that Cd activates the CaM/CaMK/NFATc1 pathway and regulates osteoclast differentiation by increasing intracellular calcium concentration. Our data provide new insights into the mechanisms underlying osteoclast differentiation following Cd exposure. This study provides a theoretical basis for future investigations into the therapeutic application of CaMK inhibitors in osteoporosis induced by Cd exposure. [ABSTRACT FROM AUTHOR]

Published

2020