NYUHSL Faculty Bibliography

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184

Cytokine & growth factor reviews. 2023:70:54-66.DOI: 10.1016/j.cytogfr.2023.03.002

Pathogenic mechanisms of glucocorticoid-induced osteoporosis

Chen, Meng; Fu, Wenyu; Xu, Huiyun; Liu, Chuan-Ju

Glucocorticoid (GC) is one of the most prescribed medicines to treat various inflammatory and autoimmune diseases. However, high doses and long-term use of GCs lead to multiple adverse effects, particularly glucocorticoid-induced osteoporosis (GIO). Excessive GCs exert detrimental effects on bone cells, including osteoblasts, osteoclasts, and osteocytes, leading to impaired bone formation and resorption. The actions of exogenous GCs are considered to be strongly cell-type and dose dependent. GC excess inhibits the proliferation and differentiation of osteoblasts and enhances the apoptosis of osteoblasts and osteocytes, eventually contributing to reduced bone formation. Effects of GC excess on osteoclasts mainly include enhanced osteoclastogenesis, increased lifespan and number of mature osteoclasts, and diminished osteoclast apoptosis, which result in increased bone resorption. Furthermore, GCs have an impact on the secretion of bone cells, subsequently disturbing the process of osteoblastogenesis and osteoclastogenesis. This review provides timely update and summary of recent discoveries in the field of GIO, with a particular focus on the effects of exogenous GCs on bone cells and the crosstalk among them under GC excess.

PMID: 36906448

ISSN: 1879-0305

CID: 5448752

Circulation. 2023:147(9):728-742.DOI: 10.1161/CIRCULATIONAHA.122.061516

Peptide Vaccine Against ADAMTS-7 Ameliorates Atherosclerosis and Postinjury Neointima Hyperplasia

Ma, Zihan; Mao, Chenfeng; Chen, Xiao; Yang, Shiyu; Qiu, Zhihua; Yu, Baoqi; Jia, Yiting; Wu, Chao; Wang, Yiyi; Wang, Yuhui; Gu, Rui; Yu, Fang; Yin, Yanhui; Wang, Xian; Xu, Qingbo; Liu, Chuanju; Liao, Yuhua; Zheng, Jingang; Fu, Yi; Kong, Wei

BACKGROUND:The metalloprotease ADAMTS-7 (a disintegrin and metalloproteinase with thrombospondin type 1 motif 7) is a novel locus associated with human coronary atherosclerosis. ADAMTS-7 deletion protects against atherosclerosis and vascular restenosis in rodents. METHODS: RESULTS: CONCLUSIONS:ATS7vac is a novel atherosclerosis vaccine that also alleviates in-stent restenosis. The application of ATS7vac would be a complementary therapeutic avenue to the current lipid-lowering strategy for atherosclerotic disease.

PMID: 36562301

ISSN: 1524-4539

CID: 5431892

Proceedings of the National Academy of Sciences of the United States of America (PNAS). 2023:120(1).DOI: 10.1073/pnas.2210442120

PGRN deficiency exacerbates, whereas a brain penetrant PGRN derivative protects, GBA1 mutation-associated pathologies and diseases

Zhao, Xiangli; Lin, Yi; Liou, Benjamin; Fu, Wenyu; Jian, Jinlong; Fannie, Venette; Zhang, Wujuan; Setchell, Kenneth D R; Grabowski, Gregory A; Sun, Ying; Liu, Chuan-Ju

Mutations in GBA1, encoding glucocerebrosidase (GCase), cause Gaucher disease (GD) and are also genetic risks in developing Parkinson's disease (PD). Currently, the approved therapies are only effective for directly treating visceral symptoms, but not for primary neuronopathic involvement in GD (nGD). Progranulin (PGRN), encoded by GRN, is a novel modifier of GCase, but the impact of PGRN in GBA1 mutation-associated pathologies in vivo remains unknown. Herein, Grn

PMID: 36574647

ISSN: 1091-6490

CID: 5409592

Journal of advanced research. 2022:41:63-75.DOI: 10.1016/j.jare.2022.01.004

Mechanical overloading induces GPX4-regulated chondrocyte ferroptosis in osteoarthritis via Piezo1 channel facilitated calcium influx

Wang, Shaoyi; Li, Weiwei; Zhang, Pengfei; Wang, Zihao; Ma, Xiaoyuan; Liu, Chuanju; Vasilev, Krasimir; Zhang, Lei; Zhou, Xiaocong; Liu, Liang; Hayball, John; Dong, Shuli; Li, Yuhua; Gao, Yuan; Cheng, Lei; Zhao, Yunpeng

INTRODUCTIONS:Excessive mechanical stress is closely associated with cell death in various conditions. Exposure of chondrocytes to excessive mechanical loading leads to a catabolic response as well as exaggerated cell death. Ferroptosis is a recently identified form of cell death during cell aging and degeneration. However, it's potential association with mechanical stress remains to be illustrated. OBJECTIVES:To identify whether excessive mechanical stress can cause ferroptosis. To explore the role of mechanical overloading in chondrocyte ferroptosis. METHODS:) mice OA model and chondrocytes cultured with high strain mechanical stress. Furthermore, the role of Piezo1 ion channel in chondrocyte ferroptosis and OA development was explored by using its inhibitor (GsMTx4) and agonist (Yoda1). Additionally, chondrocyte was cultured in calcium-free medium with mechanical stress, and ferroptosis phenotype was tested. RESULTS:Human cartilage and mouse chondrocyte experiments revealed that mechanical overloading can induce GPX4-associated ferroptosis. Conditional knockout of GPX4 in cartilage aggravated experimental OA process, while additional treatment with ferroptosis suppressor protein (FSP-1) and coenzyme Q10 (CoQ10) abated OA development in GPX4-CKO mice. In mouse OA model and chondrocyte experiments, inhibition of Piezo1 channel activity increased GPX4 expression, attenuated ferroptosis phenotype and reduced the severity of osteoarthritis. Additionally, high strain mechanical stress induced ferroptosis damage in chondrocyte was largely abolished by blocking calcium influx through calcium-free medium. CONCLUSIONS:Our findings show that mechanical overloading induces ferroptosis through Piezo1 activation and subsequent calcium influx in chondrocytes, which might provide a potential target for OA treatment.

PMCID:9637484

PMID: 36328754

ISSN: 2090-1224

CID: 5356842

International journal of molecular sciences. 2022:23(20).DOI: 10.3390/ijms232012643

Pharmacological and Therapeutic Applications of Esculetin

Garg, Sourbh Suren; Gupta, Jeena; Sahu, Debasis; Liu, Chuan-Ju

Esculetin is a coumarin compound, which belongs to the class of benzopyrone enriched in various plants such as Sonchus grandifolius, Aesculus turbinata, etc. Free radicals lead to the development of oxidative stress causing inflammation, arthritis, cancer, diabetes, fatty liver disease, etc. These further reduce the efficacy of anticancer drugs, activate inflammatory signaling pathways, degrade joints and cartilage, and disrupt the glycemic index and normal function of liver enzymes. For instance, the current treatment modalities used in arthritis such as non-steroidal anti-inflammatory drugs, disease-modifying anti-rheumatoid drugs, and lipoxygenase inhibitors present limited efficacy and adverse effects. Thus, there is a constant need to find newer and safer alternatives. Esculetin has an immense antioxidative potential thereby alleviating arthritis, diabetes, malignancies, and hepatic disorders. Structurally, esculetin contains two hydroxyl groups, which enhance its ability to function as an antioxidant by inhibiting oxidative stress in pathological conditions. Leukotriene B4 synthesis, NF-ÎºB and MPAK pathway activation, and inflammatory cytokine production are the main causes of bone and joint deterioration in arthritis, whereas esculetin treatment reverses these factors and relieves the disease condition. In contrast, lipid peroxidation caused by upregulation of TGF-Î²-mediated expression and dysfunction of antioxidant enzymes is inhibited by esculetin therapy, thus reducing liver fibrosis by acting on the PI3K/FoxO1 pathway. Therefore, targeting NF-ÎºB, pro-inflammatory cytokines, TGF-Î² and oxidative stress may be a therapeutic strategy to alleviate arthritis and liver fibrosis.

PMCID:9604018

PMID: 36293500

ISSN: 1422-0067

CID: 5358092

Annals of the rheumatic diseases. 2022:81(4):544-555.DOI: 10.1136/annrheumdis-2021-221380

Digoxin targets low density lipoprotein receptor-related protein 4 and protects against osteoarthritis

Wang, Kai-di; Ding, Xiang; Jiang, Nan; Zeng, Chao; Wu, Jing; Cai, Xian-Yi; Hettinghouse, Aubryanna; Khleborodova, Asya; Lei, Zi-Ning; Chen, Zhe-Sheng; Lei, Guang-Hua; Liu, Chuan-Ju

OBJECTIVES/OBJECTIVE:Dysregulated chondrocyte metabolism is closely associated with the pathogenesis of osteoarthritis (OA). Suppressing chondrocyte catabolism to restore cartilage homeostasis has been extensively explored, whereas far less effort has been invested toward enhancing chondrocyte anabolism. This study aimed to repurpose clinically approved drugs as potential stimulators of chondrocyte anabolism in treating OA. METHODS:Screening of a Food and Drug Administration-approved drug library; Assays for examining the chondroprotective effects of digoxin in vitro; Assays for defining the therapeutic effects of digoxin using a surgically-induced OA model; A propensity-score matched cohort study using The Health Improvement Network to examine the relationship between digoxin use and the risk of joint OA-associated replacement among patients with atrial fibrillation; identification and characterisation of the binding of digoxin to low-density lipoprotein receptor-related protein 4 (LRP4); various assays, including use of CRISPR-Cas9 genome editing to delete LRP4 in human chondrocytes, for examining the dependence on LRP4 of digoxin regulation of chondrocytes. RESULTS:Serial screenings led to the identification of ouabain and digoxin as stimulators of chondrocyte differentiation and anabolism. Ouabain and digoxin protected against OA and relieved OA-associated pain. The cohort study of 56â€‰794 patients revealed that digoxin use was associated with reduced risk of OA-associated joint replacement. LRP4 was isolated as a novel target of digoxin, and deletion of LRP4 abolished digoxin's regulations of chondrocytes. CONCLUSIONS:These findings not only provide new insights into the understanding of digoxin's chondroprotective action and underlying mechanisms, but also present new evidence for repurposing digoxin for OA.

PMID: 34853001

ISSN: 1468-2060

CID: 5065732

Nature aging. 2022:2(4):332-347.DOI: 10.1038/s43587-021-00165-w

Kindlin-2 preserves integrity of the articular cartilage to protect against osteoarthritis

Wu, Xiaohao; Lai, Yumei; Chen, Sheng; Zhou, Chunlei; Tao, Chu; Fu, Xuekun; Li, Jun; Tong, Wei; Tian, Hongtao; Shao, Zengwu; Liu, Chuanju; Chen, Di; Bai, Xiaochun; Cao, Huiling; Xiao, Guozhi

Osteoarthritis (OA) is an aging-related degenerative joint disease with a poorly defined mechanism. Here we report that kindlin-2 is highly expressed in articular chondrocytes and downregulated in the degenerated cartilage of aged mice and patients with OA. Kindlin-2 deletion in articular chondrocytes leads to spontaneous OA and exacerbates instability-induced OA lesions in adult mice. Kindlin-2 deficiency promotes mitochondrial oxidative stress and activates Stat3, leading to Runx2-mediated chondrocyte catabolism. Pharmacological inhibition of Stat3 activation or genetic ablation of Stat3 in chondrocytes reverses aberrant accumulation of Runx2 and extracellular-matrix-degrading enzymes and limits OA deteriorations caused by kindlin-2 deficiency. Deleting Runx2 in chondrocytes reverses structural changes and OA lesions caused by kindlin-2 deletion without downregulating p-Stat3. Intra-articular injection of AAV5-kindlin-2 decelerates progression of aging- and instability-induced knee joint OA in mice. Collectively, we identify a pathway consisting of kindlin-2, Stat3 and Runx2 in articular chondrocytes that is responsible for maintaining articular cartilage integrity and define a potential therapeutic target for OA.

PMID: 37117739

ISSN: 2662-8465

CID: 5465652

Cell discovery. 2022:8(1).DOI: 10.1038/s41421-021-00363-1

Targeting macrophage TFEB-14-3-3 epsilon Interface by naringenin inhibits abdominal aortic aneurysm

Jia, Yiting; Zhang, Lu; Liu, Ziyi; Mao, Chenfeng; Ma, Zihan; Li, Wenqiang; Yu, Fang; Wang, Yingbao; Huang, Yaqian; Zhang, Weizhen; Zheng, Jingang; Wang, Xian; Xu, Qingbo; Zhang, Jian; Feng, Wei; Yun, Caihong; Liu, Chuanju; Sun, Jinpeng; Fu, Yi; Cui, Qinghua; Kong, Wei

Abdominal aortic aneurysm (AAA) is a lethal cardiovascular disease, and there is no proven drug treatment for this condition. In this study, by using the Connectivity Map (CMap) approach, we explored naringenin, a naturally occurring citrus flavonoid, as a putative agent for inhibiting AAA. We then validated the prediction with two independent mouse models of AAA, calcium phosphate (CaPO₄)-induced C57BL/6J mice and angiotensin II-infused ApoE^-/- mice. Naringenin effectively blocked the formation of AAAs and the progression of established AAAs. Transcription factor EB (TFEB) is the master regulator of lysosome biogenesis. Intriguingly, the protective role of naringenin on AAA was abolished by macrophage-specific TFEB depletion in mice. Unbiased interactomics, combined with isothermal titration calorimetry (ITC) and cellular thermal shift assays (CETSAs), further revealed that naringenin is directly bound to 14-3-3 epsilon blocked the TFEB-14-3-3 epsilon interaction, and therefore promoted TFEB nuclear translocation and activation. On one hand, naringenin activated lysosome-dependent inhibition of the NLRP3 inflammasome and repressed aneurysmal inflammation. On the other hand, naringenin induced TFEB-dependent transcriptional activation of GATA3, IRF4, and STAT6 and therefore promoted reparative M2 macrophage polarization. In summary, naturally derived naringenin or macrophage TFEB activation shows promising efficacy for the treatment of AAA.

PMID: 35228523

ISSN: 2056-5968

CID: 5174252

Arthritis research & therapy. 2022:24(1).DOI: 10.1186/s13075-021-02713-6

Penfluridol targets acid sphingomyelinase to inhibit TNF signaling and is therapeutic against inflammatory autoimmune diseases

Chen, Yue-Hong; Liu, Rong-Han; Cui, Ya-Zhou; Hettinghouse, Aubryanna; Fu, Wen-Yu; Zhang, Lei; Zhang, Chen; Liu, Chuan-Ju

BACKGROUND:Penfluridol, isolated from an FDA-approved small-molecule drug library as an inhibitor of tumor necrosis factor Î± (TNFÎ±)-stimulated NF-ÎºB activation, is clinically used to treat chronic schizophrenia and related disorders. This study is aimed to investigate the therapeutic effect of penfluridol on TNFÎ±-stimulated inflammatory autoimmune diseases, particularly inflammatory arthritis. METHODS:Various in vitro studies to confirm the inhibitory effect of penfluridol on TNFÎ±-induced NF-ÎºB activity in bone marrow-derived macrophages or Raw 264.7 macrophage cell line. In vivo studies assessed the therapeutic effects of penfluridol in various disease models, including TNFÎ± transgenic mice, collagen-induced arthritis, DSS-induced colitis, and TNBS-induced colitis. Identification and characterization of the binding of penfluridol to acid sphingomyelinase using bioinformatics and drug affinity responsive target stability assay. Acid sphingomyelinase activity assays to reveal penfluridol-mediated inhibition of acid sphingomyelinase activity. siRNA knockdown experiments to illustrate the dependence of penfluridol's anti-TNF activity on acid sphingomyelinase. RESULTS:Penfluridol effectively inhibited TNFÎ±-induced NF-ÎºB activation in vitro and alleviated the severity of arthritis and colitis in vivo. Mechanistic studies revealed that penfluridol bound to acid sphingomyelinase and inhibited its activation. In addition, knockdown of acid sphingomyelinase largely abolished the inhibitory effects of penfluridol on TNFÎ±-induced inflammatory cytokine production. Furthermore, penfluridol suppressed the differentiation of spleen naive CD4+T cells to TH1 and TH17 and inhibited M1 macrophage polarization. CONCLUSION/CONCLUSIONS:This study provides the rationale for the possible innovative use of penfluridol as a newly identified small-molecule drug for TNFÎ±-driven diseases, such as inflammatory arthritis and colitis.

PMCID:8767691

PMID: 35045889

ISSN: 1478-6362

CID: 5131602

Biomaterials. 2022:281.DOI: 10.1016/j.biomaterials.2022.121370

Injectable recombinant block polymer gel for sustained delivery of therapeutic protein in post traumatic osteoarthritis

Katyal, Priya; Hettinghouse, Aubryanna; Meleties, Michael; Hasan, Sadaf; Chen, Changhong; Cui, Min; Sun, Guodong; Menon, Rajiv; Lin, Bonnie; Regatte, Ravinder; Montclare, Jin Kim; Liu, Chuan-Ju

Protein-based biomaterials offer several advantages over synthetic materials, owing to their unique stimuli-responsive properties, biocompatibility and modular nature. Here, we demonstrate that E₅C, a recombinant protein block polymer, consisting of five repeats of elastin like polypeptide (E) and a coiled-coil domain of cartilage oligomeric matrix protein (C), is capable of forming a porous networked gel at physiological temperature, making it an excellent candidate for injectable biomaterials. Combination of E₅C with Atsttrin, a chondroprotective engineered derivative of anti-inflammatory growth factor progranulin, provides a unique biochemical and biomechanical environment to protect against post-traumatic osteoarthritis (PTOA) onset and progression. E₅C gel was demonstrated to provide prolonged release of Atsttrin and inhibit chondrocyte catabolism while facilitating anabolic signaling in vitro. We also provide in vivo evidence that prophylactic and therapeutic application of Atsttrin-loaded E₅C gels protected against PTOA onset and progression in a rabbit anterior cruciate ligament transection model. Collectively, we have developed a unique protein-based gel capable of minimally invasive, sustained delivery of prospective therapeutics, particularly the progranulin-derivative Atsttrin, for therapeutic application in OA.

PMID: 35032910

ISSN: 1878-5905

CID: 5119242

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