Your search keyword '"Panxia Wang"' showing total 39 results

1. YAP K236 acetylation facilitates its nucleic export and deprived the protection against cardiac hypertrophy in mice

Author

Panxia Wang, Luping Wang, Cui Liu, Yuehuai Hu, Guodong Feng, Zuqian Lian, Jing Lu, Ping He, Hexin Cai, Xiaohui Liang, Peiqing Liu, and Xiaoqian Wu

Subjects

Cardiac hypertrophy, YAP, K236 residues, Acetylation, SIRT6, Therapeutics. Pharmacology, RM1-950

Abstract

The subcellular localization of Yes-associated protein (YAP) is dynamically regulated by post-transcriptional modifications, critically influencing cardiac function. Despite its significance, the precise mechanism controlling YAP nuclear sequestration and its role in cardiac hypertrophy remain poorly defined. In this study, utilizing immunoprecipitation-mass spectrometry, we identified potential acetylation sites and interacting proteins of YAP. Co-immunoprecipitation and immunofluorescence assays were used to elucidate the protein interactions and subcellular colocalization. We found that YAP protected against ISO-induced pathological cardiac hypertrophy both in vivo and in vitro. During cardiac hypertrophy YAP acetylation increased while its nuclear accumulation reduced without altering Ser127 phosphorylation. Notably, lysine 236 was identified as a novel acetylation site on YAP. Acetylation at K236 facilitated YAP’s nucleic export, suppressed the expression of target genes such as NRF1 and Cox IV, and counteracted YAP's anti-hypertrophic effects. Importantly, deacetylase SIRT6 was identified as a regulator of YAP deacetylation, disrupting the YAP with chaperone protein 14–3–3 interaction and inhibiting YAP’s nuclear export, thereby facilitating cardiac protective role of YAP. This study identified YAP K236 acetylation as a key regulator of its nuclear retention in cardiomyocytes, with SIRT6-mediated deacetylation facilitating YAP’s protective effects against cardiac hypertrophy. Targeting YAP acetylation may offer a promising therapeutic strategy for cardiac hypertrophy.

Published

2025

2. Sorting nexin 3 exacerbates doxorubicin-induced cardiomyopathy via regulation of TFRC-dependent ferroptosis

Author

Wenjing Yu, Yuehuai Hu, Zhiping Liu, Kaiteng Guo, Dinghu Ma, Mingxia Peng, Yuemei Wang, Jing Zhang, Xiaolei Zhang, Panxia Wang, Jiguo Zhang, Peiqing Liu, and Jing Lu

Subjects

SNX3, Ferroptosis, TFRC, Cardiomyopathy, Doxorubicin, Iron homeostasis, Therapeutics. Pharmacology, RM1-950

Abstract

The clinical utilization of doxorubicin (Dox) in various malignancies is restrained by its major adverse effect: irreversible cardiomyopathy. Extensive studies have been done to explore the prevention of Dox cardiomyopathy. Currently, ferroptosis has been shown to participate in the incidence and development of Dox cardiomyopathy. Sorting Nexin 3 (SNX3), the retromer-associated cargo binding protein with important physiological functions, was identified as a potent therapeutic target for cardiac hypertrophy in our previous study. However, few study has shown whether SNX3 plays a critical role in Dox-induced cardiomyopathy. In this study, a decreased level of SNX3 in Dox-induced cardiomyopathy was observed. Cardiac-specific Snx3 knockout (Snx3-cKO) significantly alleviated cardiomyopathy by downregulating Dox-induced ferroptosis significantly. SNX3 was further demonstrated to exacerbate Dox-induced cardiomyopathy via induction of ferroptosis in vivo and in vitro, and cardiac-specific Snx3 transgenic (Snx3-cTg) mice were more susceptible to Dox-induced ferroptosis and cardiomyopathy. Mechanistically, SNX3 facilitated the recycling of transferrin 1 receptor (TFRC) via direct interaction, disrupting iron homeostasis, increasing the accumulation of iron, triggering ferroptosis, and eventually exacerbating Dox-induced cardiomyopathy. Overall, these findings established a direct SNX3–TFRC–ferroptosis positive regulatory axis in Dox-induced cardiomyopathy and suggested that targeting SNX3 provided a new effective therapeutic strategy for Dox-induced cardiomyopathy through TFRC-dependent ferroptosis.

Published

2023

3. Cryptotanshinone attenuates LPS-induced acute lung injury by regulating metabolic reprogramming of macrophage

Author

Zesen Ye, Panxia Wang, Guodong Feng, Quan Wang, Cui Liu, Jing Lu, Jianwen Chen, and Peiqing Liu

Subjects

acute lung injury, Cryptotanshinone, macrophage polarization, metabolic reprogramming, AMPK, Medicine (General), R5-920

Abstract

BackgroundAcute lung injury (ALI) is a life-threatening inflammatory disease without effective therapeutic regimen. Macrophage polarization plays a key role in the initiation and resolution of pulmonary inflammation. Therefore, modulating macrophage phenotype is a potentially effective way for acute lung injury. Cryptotanshinone (CTS) is a lipophilic bioactive compound extracted from the root of Salvia miltiorrhiza with a variety of pharmacological effects, especially the anti-inflammatory role. In this study, we investigated the therapeutic and immunomodulatory effects of CTS on ALI.Materials and methodsThe rat model of ALI was established by intratracheal instillation of LPS (5 mg/kg) to evaluate the lung protective effect of CTS in vivo and to explore the regulation of CTS on the phenotype of lung macrophage polarization. LPS (1 μg/mL) was used to stimulate RAW264.7 macrophages in vitro to further explore the effect of CTS on the polarization and metabolic reprogramming of RAW264.7 macrophages and to clarify the potential mechanism of CTS anti-ALI.ResultsCTS significantly improved lung function, reduced pulmonary edema, effectively inhibited pulmonary inflammatory infiltration, and alleviated ALI. Both in vivo and in vitro results revealed that CTS inhibited the differentiation of macrophage into the M1 phenotype and promoted polarization into M2 phenotype during ALI. Further in vitro studies indicated that CTS significantly suppressed LPS-induced metabolic transition from aerobic oxidation to glycolysis in macrophages. Mechanistically, CTS blocked LPS-induced metabolic transformation of macrophages by activating AMPK.ConclusionThese findings demonstrated that CTS regulates macrophage metabolism by activating AMPK, and then induced M1-type macrophages to transform into M2-type macrophages, thereby alleviating the inflammatory response of ALI, suggesting that CTS might be a potential anti-ALI agent.

Published

2023

4. Trypsin inhibitor LH011 inhibited DSS-induced mice colitis via alleviating inflammation and oxidative stress

Author

Zhenmao Jia, Panxia Wang, Yuansheng Xu, Guodong Feng, Quan Wang, Xiangjun He, Yan Song, Peiqing Liu, and Jianwen Chen

Subjects

UC, LH011, inflammation, oxidative stress, NF-κB, Nrf2, Therapeutics. Pharmacology, RM1-950

Abstract

Background: Ulcerative colitis (UC) is one type of inflammatory bowel disease, characterized by inflammation with infiltration and activation of macrophages in colonic tissue. LH011 is a trypsin inhibitor with potential anti-inflammatory effect.Purpose: Here, we aim to assay the effects of LH011 on UC and further investigate the potential mechanisms in vitro and in vivo.Methods: Dextran sulfate sodium (DSS, 3.5%, w/v) was used to induce UC, and lipopolysaccharide (LPS) was used to induce inflammation in RAW 264.7 cells. LH011 was administrated to mice in vivo or to RAW 264.7 cells in vitro at different concentrations. The cytokines (IL-1β, IL-6, and TNF-α) and the changes of NF-κB and Nrf2 pathways were detected.Results: The results showed that LH011 improved DSS-induced mice colitis, including loss of weight, disease activity index (DAI), and colonic pathological damage. In addition, LH011 inhibited the expressions of IL-1β, IL-6, and TNF-α and strengthened the anti-oxidative capacity. Mechanically, LH011 downregulated the nuclear localization of NF-κB p65 and upregulated the protein expression of Nrf2.Conclusion: These results demonstrated that LH011 alleviated inflammation and oxidative stress during UC by inhibiting TLR4/NF-κB and activating Nrf2/Keap1/HO-1 signaling pathways.

Published

2022

5. Isorhapontigenin protects against doxorubicin-induced cardiotoxicity via increasing YAP1 expression

Author

Panxia Wang, Minghui Wang, Yuehuai Hu, Jianxing Chen, Yanjun Cao, Cui Liu, Zhongkai Wu, Juan Shen, Jing Lu, and Peiqing Liu

Subjects

Isorhapontigenin, YAP1, Doxorubicin, Cardiotoxicity, Cardiomyocytes apoptosis, TEAD1, Therapeutics. Pharmacology, RM1-950

Abstract

As an effective anticancer drug, the clinical limitation of doxorubicin (Dox) is the time- and dose-dependent cardiotoxicity. Yes-associated protein 1 (YAP1) interacts with transcription factor TEA domain 1 (TEAD1) and plays an important role in cell proliferation and survival. However, the role of YAP1 in Dox-induced cardiomyopathy has not been reported. In this study, the expression of YAP1 was reduced in clinical human failing hearts with dilated cardiomyopathy and Dox-induced in vivo and in vitro cardiotoxic model. Ectopic expression of Yap1 significantly blocked Dox-induced cardiomyocytes apoptosis in TEAD1 dependent manner. Isorhapontigenin (Isor) is a new derivative of stilbene and responsible for a wide range of biological processes. Here, we found that Isor effectively relieved Dox-induced cardiomyocytes apoptosis in a dose-dependent manner in vitro. Administration with Isor (30 mg/kg/day, intraperitoneally, 3 weeks) significantly protected against Dox-induced cardiotoxicity in mice. Interestingly, Isor increased Dox-caused repression in YAP1 and the expression of its target genes in vivo and in vitro. Knockout or inhibition of Yap1 blocked the protective effects of Isor on Dox-induced cardiotoxicity. In conclusion, YAP1 may be a novel target for Dox-induced cardiotoxicity and Isor might be a new compound to fight against Dox-induced cardiotoxicity by increasing YAP1 expression.

Published

2021

6. Targeting castration-resistant prostate cancer with a novel RORγ antagonist elaiophylin

Author

Jianwei Zheng, Junfeng Wang, Qian Wang, Hongye Zou, Hong Wang, Zhenhua Zhang, Jianghe Chen, Qianqian Wang, Panxia Wang, Yueshan Zhao, Jing Lu, Xiaolei Zhang, Songtao Xiang, Haibin Wang, Jinping Lei, Hong-Wu Chen, Peiqing Liu, Yonghong Liu, Fanghai Han, and Junjian Wang

Subjects

RORγ, Castration-resistant prostate cancer, Nuclear receptor, Antagonist, Elaiophylin, Therapeutics. Pharmacology, RM1-950

Abstract

Prostate cancer (PCa) patients who progress to metastatic castration-resistant PCa (mCRPC) mostly have poor outcomes due to the lack of effective therapies. Our recent study established the orphan nuclear receptor RORγ as a novel therapeutic target for CRPC. Here, we reveal that elaiophylin (Elai), an antibiotic from Actinomycete streptomyces, is a novel RORγ antagonist and showed potent antitumor activity against CRPC in vitro and in vivo. We demonstrated that Elai selectively binded to RORγ protein and potently blocked RORγ transcriptional regulation activities. Structure–activity relationship studies showed that Elai occupied the binding pocket with several key interactions. Furthermore, Elai markedly reduced the recruitment of RORγ to its genomic DNA response element (RORE), suppressed the expression of RORγ target genes AR and AR variants, and significantly inhibited PCa cell growth. Importantly, Elai strongly suppressed tumor growth in both cell line based and patient-derived PCa xenograft models. Taken together, these results suggest that Elai is novel therapeutic RORγ inhibitor that can be used as a drug candidate for the treatment of human CRPC.

Published

2020

7. Chrysophanol protects against doxorubicin-induced cardiotoxicity by suppressing cellular PARylation

Author

Jing Lu, Jingyan Li, Yuehuai Hu, Zhen Guo, Duanping Sun, Panxia Wang, Kaiteng Guo, Dayue Darrel Duan, Si Gao, Jianmin Jiang, Junjian Wang, and Peiqing Liu

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

The clinical application of doxorubicin (DOX) in cancer chemotherapy is limited by its life-threatening cardiotoxic effects. Chrysophanol (CHR), an anthraquinone compound isolated from the rhizome of Rheum palmatum L., is considered to play a broad role in a variety of biological processes. However, the effects of CHR׳s cardioprotection in DOX-induced cardiomyopathy is poorly understood. In this study, we found that the cardiac apoptosis, mitochondrial injury and cellular PARylation levels were significantly increased in H9C2 cells treated by Dox, while these effects were suppressed by CHR. Similar results were observed when PARP1 activity was suppressed by its inhibitors 3-aminobenzamide (3AB) and ABT888. Ectopic expression of PARP1 effectively blocked this CHR׳s cardioprotection against DOX-induced cardiomyocyte injury in H9C2 cells. Furthermore, pre-administration with both CHR and 3AB relieved DOX-induced cardiac apoptosis, mitochondrial impairment and heart dysfunction in Sprague–Dawley rat model. These results revealed that CHR protects against DOX-induced cardiotoxicity by suppressing cellular PARylation and provided critical evidence that PARylation may be a novel target for DOX-induced cardiomyopathy. KEY WORDS: Chrysophanol, Doxorubicin, PARylation, Cardiotoxicity, Apoptosis, Mitochondria

Published

2019

8. PRMT5 Prevents Cardiomyocyte Hypertrophy via Symmetric Dimethylating HoxA9 and Repressing HoxA9 Expression

Author

Sidong Cai, Rong Liu, Panxia Wang, Jingyan Li, Tingting Xie, Minghui Wang, Yanjun Cao, Zhuoming Li, and Peiqing Liu

Subjects

protein arginine methyltransferase 5, homebox A9, cardiomyocyte hypertrophy, symmetric dimethylation, brain natriuretic peptide, Therapeutics. Pharmacology, RM1-950

Abstract

The present study reveals a link between protein arginine methyltransferase 5 (PRMT5) and Homebox A9 (HoxA9) in the regulation of cardiomyocyte hypertrophy. In cardiomyocyte hypertrophy induced by β-adrenergic receptor agonist isoprenaline (ISO), PRMT5 expression was decreased while HoxA9 was upregulated. Silencing of PRMT5 or inhibition of PRMT5 by its pharmacological inhibitor EPZ augmented the expressions of cardiomyocyte hypertrophic genes brain natriuretic peptide (BNP) and β-Myosin Heavy Chain (β-MHC), whereas overexpression of PRMT5 inhibited ISO-induced cardiomyocyte hypertrophy, suggesting that PRMT5 ameliorates cardiomyocyte hypertrophy. On the contrary, HoxA9 promoted cardiomyocyte hypertrophy, as implied by the gain-of-function and loss-of-function experiments. HoxA9 was involved in the regulation of PRMT5 in cardiomyocyte hypertrophy, since HoxA9 knockdown prevented si-RPMT5-induced cardiomyocyte hypertrophy, and HoxA9 expression impaired the anti-hypertrophic effect of PRMT5. Co-immunoprecipitation experiments revealed that there were physical interactions between PRMT5 and HoxA9. The symmetric dimethylation level of HoxA9 was decreased by ISO or EPZ treatment, suggesting that HoxA9 is methylated by PRMT5. Additionally, PRMT5 repressed the expression of HoxA9. Chromatin immunoprecipitation (ChIP) assay demonstrated that HoxA9 could bind to the promoter of BNP, and that this binding affinity was further enhanced by ISO or EPZ. In conclusion, this study suggests that PRMT5 symmetric dimethylates HoxA9 and represses HoxA9 expression, thus impairing its binding to BNP promoter and ultimately protecting against cardiomyocyte hypertrophy. These findings provide a novel insight of the mechanism underlying the cardiac protective effect of PRMT5, and suggest potential therapeutic strategies of PRMT5 activation or HoxA9 inhibition in treatment of cardiac hypertrophy.

Published

2020

9. Histone Demethylase JMJD3 Mediated Doxorubicin-Induced Cardiomyopathy by Suppressing SESN2 Expression

Author

Panxia Wang, Rui Lan, Zhen Guo, Sidong Cai, Junjian Wang, Quan Wang, Zeyu Li, Zhenzhen Li, Qianqian Wang, Jingyan Li, Zhongkai Wu, Jing Lu, and Peiqing Liu

Subjects

JMJD3, histone modification, SESN2, cardiotoxicity, H3K27me3, Biology (General), QH301-705.5

Abstract

Jumonji domain-containing 3 (JMJD3) protein, a histone demethylase protein, specifically catalyzes the demethylation of H3K27 (H3K27me3) and regulates gene expression. Sestrin2 (SESN2), a stress-inducible protein, protected against doxorubicin (DOX)-induced cardiomyopathy by regulating mitophagy and mitochondrial function. Here, the expression of JMJD3 was increased and that of SESN2 was decreased in both the heart samples from patients with dilated cardiomyopathy and chronic DOX-stimulation induced cardiomyopathy. Inhibition or knockdown of JMJD3 attenuated DOX-induced cardiomyocytes apoptosis, mitochondrial injury and cardiac dysfunction. However, JMJD3 overexpression aggravated DOX-induced cardiomyopathy, which were relieved by SESN2 overexpression. JMJD3 inhibited the transcription of SESN2 by reducing tri-methylation of H3K27 in the promoter region of SESN2. In conclusion, JMJD3 negatively regulated SESN2 via decreasing H3K27me3 enrichment in the promoter region of SESN2, subsequently inducing mitochondrial dysfunction and cardiomyocytes apoptosis. Targeting the JMJD3-SESN2 signaling axis may be a potential therapeutic strategy to protect against DOX-mediated cardiomyopathy.

Published

2020

10. PKCζ interacts with STAT3 and promotes its activation in cardiomyocyte hypertrophy

Author

Jingyan Li, Hui Gao, Junying Huang, Panxia Wang, Yi Huang, Wenwei Luo, Xiaoying Zhang, Peiye Shen, Jia You, Sidong Cai, Zhuoming Li, and Peiqing Liu

Subjects

Cardiac hypertrophy, Phenylephrine, PKCζ, STAT3, Phosphorylation, Therapeutics. Pharmacology, RM1-950

Abstract

This study was aimed to investigate the crosstalk between protein kinase C ζ (PKCζ) and signal transducer and activator of transcription 3 (STAT3) in cardiomyocyte hypertrophy. In neonatal rat cardiomyocyte hypertrophic model induced by phenylephrine (PE), the levels of phosphorylated PKCζ and phosphorylated STAT3 were significantly increased, suggesting the activation of both PKCζ and STAT3 in cardiomyocyte hypertrophy. Overexpression of PKCζ by adenovirus infection elevated the expressions of hypertrophic markers atrial natriuretic factor (ANF) and brains natriuretic polypeptide (BNP), as well as the cell surface area; while genetic silencing of PKCζ inhibited PE-induced cardiomyocyte hypertrophy. An interaction between PKCζ and STAT3 in cardiomyocytes was shown by co-immunoprecipitation experiments. Overexpression of PKCζ increased the phosphorylated level of STAT3 at both Ser727 and Tyr705, promoted the nuclear translocation of STAT3, and enhanced the expression of STAT3 downstream target genes c-fos and angiotensinogen (aGT); whereas PKCζ knockdown prevented PE-induced STAT3 activation, nuclear shuttling and transcriptional activation. In conclusion, PKCζ interacts with STAT3 and promotes its activation in cardiomyocyte hypertrophy. Strategies targeting inhibition of PKCζ-STAT3 signaling pathway suggest a therapeutic potential for cardiac hypertrophy.

Published

2016

11. SIRT6 Suppresses NFATc4 Expression and Activation in Cardiomyocyte Hypertrophy

Author

Zhenzhen Li, Xiaoying Zhang, Zhen Guo, Yao Zhong, Panxia Wang, Jingyan Li, Zhuoming Li, and Peiqing Liu

Subjects

cardiomyocyte hypertrophy, SIRT6, deacetylase activity, NFATc4, BNP, Therapeutics. Pharmacology, RM1-950

Abstract

NFATc4, a member from the Nuclear Factor of Activated T cells (NFATs) transcription factor family, plays a pivotal role in the development of cardiac hypertrophy. NFATc4 is dephosphorylated by calcineurin and translocated from the cytoplasm to the nucleus to regulate the expression of hypertrophic genes, like brain natriuretic polypeptide (BNP). The present study identified SIRT6, an important subtype of NAD+ dependent class III histone deacetylase, to be a negative regulator of NFATc4 in cardiomyocyte hypertrophy. In phenylephrine (PE)-induced hypertrophic cardiomyocyte model, overexpression of SIRT6 by adenovirus infection or by plasmid transfection repressed the protein and mRNA expressions of NFATc4, elevated its phosphorylation level, prevented its nuclear accumulation, subsequently suppressed its transcriptional activity and downregulated its target gene BNP. By contrast, mutant of SIRT6 without deacetylase activity (H133Y) did not demonstrate these effects, suggesting that the inhibitory effect of SIRT6 on NFATc4 was dependent on its deacetylase activity. Moreover, the effect of SIRT6 overexpression on repressing BNP expression was reversed by NFATc4 replenishment, whereas the effect of SIRT6 deficiency on upregulating BNP was recovered by NFATc4 silencing. Mechanistically, interactions between SIRT6 and NFATc4 might possibly facilitate the deacetylation of NFATc4 by SIRT6, thereby preventing the activation of NFATc4. In conclusion, the present study reveals that SIRT6 suppresses the expression and activation of NFATc4. These findings provide more evidences of the anti-hypertrophic effect of SIRT6 and suggest SIRT6 as a potential therapeutic target for cardiac hypertrophy.

Published

2019

12. The cross-talk between PARylation and SUMOylation in C/EBPβ at K134 site participates in pathological cardiac hypertrophy

Author

Luping Wang, Panxia Wang, Suowen Xu, Zhuoming Li, Dayue Darrel Duan, Jiantao Ye, Jingyan Li, Yanqing Ding, Wenqing Zhang, Jing Lu, and Peiqing Liu

Subjects

Male, CCAAT-Enhancer-Binding Protein-beta, cardiac hypertrophy, SUMO-1 Protein, poly(ADP-ribosyl)ation, Poly (ADP-Ribose) Polymerase-1, Sumoylation, Cardiomegaly, Cell Biology, Applied Microbiology and Biotechnology, Rats, Rats, Sprague-Dawley, Disease Models, Animal, HEK293 Cells, C/EBPβ, Animals, Humans, Protein Processing, Post-Translational, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Protein Binding, Research Paper, Developmental Biology

Abstract

Poly(ADP-ribosyl)ation (PARylation) and SUMO modification (SUMOylation) are novel post-translational modifications (PTMs) mainly induced by PARP1 and SUMO1. Growing evidence has revealed that C/EBPβ plays multiple roles in biological processes and participates in cardiovascular diseases. However, the cross-talk between C/EBPβ PARylation and SUMOylation during cardiovascular diseases is unknown. This study aims to investigate the effects of C/EBPβ PTMs on cardiac hypertrophy and its underlying mechanism. Abdominal aortic constriction (AAC) and phenylephrine (PE) were conducted to induce cardiac hypertrophy. Intramyocardial delivery of recombinant adenovirus (Ad-PARP1) was taken to induce PARP1 overexpression. In this study, we found C/EBPβ participates in PARP1-induced cardiac hypertrophy. C/EBPβ K134 residue could be both PARylated and SUMOylated individually by PARP1 and SUMO1. Moreover, the accumulation of PARylation on C/EBPβ at K134 site exhibits downregulation of C/EBPβ SUMOylation at the same site. Importantly, C/EBPβ K134 site SUMOylation could decrease C/EBPβ protein stability and participates in PARP1-induced cardiac hypertrophy. Taken together, these findings highlight the importance of the cross-talk between C/EBPβ PTMs at K134 site in determining its protein level and function, suggesting that multi-target pharmacological strategies inhibiting PARP1 and activating C/EBPβ SUMOylation would be potential for treating pathological cardiac hypertrophy.

Published

2022

13. SNX3 aggravates pathological cardiac hypertrophy via targeting ATG5-dependent autophagy

Author

Yuehuai Hu, Panxia Wang, Jianxing Chen, Cui Liu, Wenjing Yu, Zhongkai Wu, Jing Lu, and Peiqing Liu

Abstract

Autophagy is an intracellular lysosomal degradation pathway that plays a critical role in maintaining cardiac homeostasis. Disordered autophagy is closely related to the pathological process of many heart diseases, including cardiac hypertrophy. However, mechanisms regulating cardiac autophagy remained unclear. Previously, we found that overexpression of SNX3 induces cardiac hypertrophy in mice. In this study, a reduced autophagy was observed in SNX3 transgenic mice. Therefore, the objective of our study was to determine whether SNX3 regulates pathological cardiac hypertrophy by regulating autophagy process. A decreased level of autophagy-related protein LC3 was detected in failing hearts from human patients and mouse models. To explore the role of SNX3 in cardiac autophagy, we generated cardiac-specific SNX3 transgenic mice and infected neonatal rat cardiomyocytes (NRCMs) with adenovirus encoding SNX3 (Ad-SNX3). Both in vivo and in vitro studies suggested that overexpression of SNX3 inhibited cardiomyocytes autophagy. Overexpression of SNX3 in vitro further reduced ISO-induced autophagic flux through inhibiting autophagic formation. Rapamycin, an autophagy inducer, could effectively reversed SNX3-induced cardiac hypertrophy and autophagy inhibition both in vitro and in vivo. Immunofluorescent staining and co-immunoprecipitation results revealed an interaction between SNX3 and autophagy related gene 5 (ATG5). We discovered that the stability of ATG5 was impaired by SNX3.

Published

2022

14. Isorhapontigenin protects against doxorubicin-induced cardiotoxicity via increasing YAP1 expression

Author

Jian-Xing Chen, Jing Lu, Yanjun Cao, Yuehuai Hu, Zhongkai Wu, Peiqing Liu, Cui Liu, Minghui Wang, Panxia Wang, and Juan Shen

Subjects

Isorhapontigenin, YAP1, Pharmacology, Cardiomyocytes apoptosis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Amphiregulin, polycyclic compounds, medicine, Doxorubicin, TEAD1, General Pharmacology, Toxicology and Pharmaceutics, 030304 developmental biology, 0303 health sciences, Cardiotoxicity, lcsh:RM1-950, technology, industry, and agriculture, carbohydrates (lipids), lcsh:Therapeutics. Pharmacology, chemistry, Apoptosis, 030220 oncology & carcinogenesis, Ectopic expression, medicine.drug

Abstract

As an effective anticancer drug, the clinical limitation of doxorubicin (Dox) is the time- and dose-dependent cardiotoxicity. Yes-associated protein 1 (YAP1) interacts with transcription factor TEA domain 1 (TEAD1) and plays an important role in cell proliferation and survival. However, the role of YAP1 in Dox-induced cardiomyopathy has not been reported. In this study, the expression of YAP1 was reduced in clinical human failing hearts with dilated cardiomyopathy and Dox-induced in vivo and in vitro cardiotoxic model. Ectopic expression of Yap1 significantly blocked Dox-induced cardiomyocytes apoptosis in TEAD1 dependent manner. Isorhapontigenin (Isor) is a new derivative of stilbene and responsible for a wide range of biological processes. Here, we found that Isor effectively relieved Dox-induced cardiomyocytes apoptosis in a dose-dependent manner in vitro. Administration with Isor (30 mg/kg/day, intraperitoneally, 3 weeks) significantly protected against Dox-induced cardiotoxicity in mice. Interestingly, Isor increased Dox-caused repression in YAP1 and the expression of its target genes in vivo and in vitro. Knockout or inhibition of Yap1 blocked the protective effects of Isor on Dox-induced cardiotoxicity. In conclusion, YAP1 may be a novel target for Dox-induced cardiotoxicity and Isor might be a new compound to fight against Dox-induced cardiotoxicity by increasing YAP1 expression.

Published

2021

15. MicroRNA-99b-3p promotes angiotensin II-induced cardiac fibrosis in mice by targeting GSK-3β

Author

Yanqing Ding, Hang Zhou, Jing Yuan, Jiantao Ye, Xueying Bi, Youhui Yu, Panxia Wang, Li-li Zhang, and Yuhong Zhang

Subjects

Male, 0301 basic medicine, Cardiac fibrosis, Cardiomyopathy, Pharmacology, Article, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, Fibrosis, medicine, Animals, Pharmacology (medical), Antagomir, 3' Untranslated Regions, Gene knockdown, Glycogen Synthase Kinase 3 beta, business.industry, Angiotensin II, Myocardium, Antagomirs, General Medicine, Fibroblasts, medicine.disease, Up-Regulation, Mice, Inbred C57BL, MicroRNAs, 030104 developmental biology, chemistry, Cardiovascular Diseases, 030220 oncology & carcinogenesis, Heart failure, business

Abstract

Cardiac fibrosis is a typical pathological change in various cardiovascular diseases. Although it has been recognized as a crucial risk factor responsible for heart failure, there is still a lack of effective treatment. Recent evidence shows that microRNAs (miRNAs) play an important role in the development of cardiac fibrosis and represent novel therapeutic targets. In this study we tried to identify the cardiac fibrosis-associated miRNA and elucidate its regulatory mechanisms in mice. Cardiac fibrosis was induced by infusion of angiotensin II (Ang II, 2 mg·kg(−1)·d(−1)) for 2 weeks via osmotic pumps. We showed that Ang II infusion induced cardiac disfunction and fibrosis accompanied by markedly increased expression level of miR-99b-3p in heart tissues. Upregulation of miR-99b-3p and fibrotic responses were also observed in cultured rat cardiac fibroblasts (CFs) treated with Ang II (100 nM) in vitro. Transfection with miR-99b-3p mimic resulted in the overproduction of fibronectin, collagen I, vimentin and α-SMA, and facilitated the proliferation and migration of CFs. On the contrary, transfection with specific miR-99b-3p inhibitor attenuated Ang II-induced fibrotic responses. Similarly, intravenous injection of specific miR-99b-3p antagomir could prevent Ang II-infused mice from cardiac dysfunction and fibrosis. We identified glycogen synthase kinase-3 beta (GSK-3β) as a direct target of miR-99b-3p. In CFs, miR-99b-3p mimic significantly reduced the expression of GSK-3β, leading to activation of its downstream profibrotic effector Smad3, whereas miR-99b-3p inhibitor caused anti-fibrotic effects. GSK-3β knockdown ameliorated the anti-fibrotic role of miR-99b-3p inhibitor. These results suggest that miR-99b-3p contributes to Ang II-induced cardiac fibrosis at least partially through GSK-3β. The modulation of miR-99b-3p may provide a new approach for tackling fibrosis-related cardiomyopathy.

Published

2020

16. sFRP1 protects H9c2 cardiac myoblasts from doxorubicin-induced apoptosis by inhibiting the Wnt/PCP-JNK pathway

Author

Yuehuai Hu, Fanghai Han, Panxia Wang, Jian-Xing Chen, Junjian Wang, Jing Lu, Peiqing Liu, Ying Guo, Jie Liu, and Wei Li

Subjects

Male, 0301 basic medicine, Cell, Antineoplastic Agents, doxorubicin, Article, Cell Line, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, sFRP1, In vivo, polycyclic compounds, medicine, Animals, Pharmacology (medical), Doxorubicin, Viability assay, Wnt Signaling Pathway, Anthracenes, Pharmacology, SP600125, Cardiotoxicity, Chemistry, Kinase, Wnt/PCP-JNK pathway, apoptosis, JNK Mitogen-Activated Protein Kinases, Wnt signaling pathway, Membrane Proteins, General Medicine, 030104 developmental biology, medicine.anatomical_structure, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Intercellular Signaling Peptides and Proteins, Wnt/β-catenin signaling, medicine.drug

Abstract

Doxorubicin (Dox) is an effective chemotherapy drug against a wide range of cancers, including both hematological and solid tumors. However, the serious cardiotoxic effect restricted its clinical application. We previously have illuminated the protective role of canonical Wnt/β-catenin signaling in Dox-induced cardiotoxicity. Secreted frizzled-related protein 1 (sFRP1) is one of the endogenous inhibitors of both canonical and noncanonical Wnt signaling. In this study, we investigated the relationship between sFRP1 and noncanonical Wnt/PCP-JNK (Wnt/planar cell polarity-c-Jun N-terminal kinase) pathway in Dox-induced cardiotoxicity in vitro and in vivo. We showed that treatment of H9c2 cardiac myoblasts with Dox (1 μM) time-dependently suppressed cell viability accompanied by significantly decreased sFRP1 protein level and increased Wnt/PCP-JNK signaling. Pretreatment with SP600125, the Wnt/PCP-JNK signaling inhibitor, attenuated Dox-induced apoptosis of H9c2 cells. Overexpression of sFRP1 protected H9c2 cells from Dox-induced apoptosis by inhibiting the Wnt/PCP-JNK pathway. After intraperitoneal injection of a cumulative dose of 15 mg/kg Dox, rats displayed significant cardiac dysfunction; their heart showed inhibited Wnt/β-catenin signaling and activated Wnt/PCP-JNK signaling. These results suggest that sFRP1 may be a novel target for Dox-induced cardiotoxicity.

Published

2020

17. SESN2 protects against doxorubicin-induced cardiomyopathy via rescuing mitophagy and improving mitochondrial function

Author

Junjian Wang, Juan Shen, Panxia Wang, Luping Wang, Kaiteng Guo, Qianqian Wang, Jiyan Xie, Zhenzhen Li, Yuehuai Hu, Sidong Cai, Rui Lan, Jing Lu, Liying Liang, and Peiqing Liu

Subjects

Male, 0301 basic medicine, FIS1, Mitochondrial disease, Gene Dosage, MFN2, Apoptosis, Mice, Transgenic, PINK1, 030204 cardiovascular system & hematology, Models, Biological, Parkin, Rats, Sprague-Dawley, 03 medical and health sciences, Adenosine Triphosphate, 0302 clinical medicine, Mitophagy, polycyclic compounds, medicine, Animals, MFN1, Myocytes, Cardiac, Molecular Biology, Membrane Potential, Mitochondrial, Cardiotoxicity, business.industry, medicine.disease, Mitochondria, Rats, Cell biology, carbohydrates (lipids), Disease Models, Animal, Genes, Mitochondrial, 030104 developmental biology, Peroxidases, Doxorubicin, Cardiomyopathies, Cardiology and Cardiovascular Medicine, business

Abstract

The clinical application of doxorubicin (Dox) in cancer therapy is limited by its serious cardiotoxicity. Our previous studies and others have recognized that mitochondrial dysfunction is the common feature of Dox-induced cardiotoxicity. However, mechanisms underlying mitochondrial disorders remained largely unknown. SESN2, a highly conserved and stress-inducible protein, is involved in mitochondrial function and autophagy in cardiovascular diseases. This study aimed to investigate whether SESN2 affects Dox-induced cardiotoxicity and the underlying mechanisms. Sprague-Dawley rats and neonatal rat cardiomyocytes were treated with Dox. SESN2 expression was assessed. The effects of SESN2 on Dox-induced cardiotoxicity were assessed by functional gain and loss experiments. Echocardiographic parameters, morphological and histological analyses, transmission electron microscope and immunofluorescence assays were used to assess cardiac and mitochondrial function. The protein expression of SESN2 was significantly reduced following Dox stimulation. Both knockout of SESN2 by sgRNA and Dox treatment resulted in the inhibition of Parkin-mediated mitophagy, marked cardiomyocytes apoptosis and mitochondria dysfunction. Ectopic expression of SESN2 effectively protected against Dox-induced cardiomyocyte apoptosis, mitochondrial injury and cardiac dysfunction. Mechanistically, SESN2 interacted with Parkin and p62, promoted accumulation of Parkin to mitochondria and then alleviated Dox-caused inhibition of Parkin mediated mitophagy. Ultimately, the clearance of damaged mitochondria and mitochondrial function were improved following SESN2 overexpression. SESN2 protected against Dox-induced cardiotoxicity through improving mitochondria function and mitophagy. These results established SESN2 as a key player in mitochondrial function and provided a potential therapeutic approach to Dox-induced cardiomyopathy.

Published

2019

18. The Cross-Talk Between PARylation and SUMOylation in C/EBPβ at K134 Site Participates in Pathological Cardiac Hypertrophy

Author

Luping Wang, Panxia Wang, Jing Lu, Zhuoming Li, Dayue Darrel Duan, Jiantao Ye, Jingyan Li, Yanqing Ding, and Peiqing Liu

Published

2021

19. PRMT5 Prevents Cardiomyocyte Hypertrophy via Symmetric Dimethylating HoxA9 and Repressing HoxA9 Expression

Author

Rong Liu, Panxia Wang, Jingyan Li, Minghui Wang, Tingting Xie, Peiqing Liu, Sidong Cai, Yanjun Cao, and Zhuoming Li

Subjects

0301 basic medicine, cardiomyocyte hypertrophy, 030204 cardiovascular system & hematology, brain natriuretic peptide, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Isoprenaline, medicine, Gene silencing, Pharmacology (medical), Receptor, protein arginine methyltransferase 5, Original Research, Pharmacology, Gene knockdown, Chemistry, Protein arginine methyltransferase 5, lcsh:RM1-950, symmetric dimethylation, Brain natriuretic peptide, Cell biology, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, homebox A9, Chromatin immunoprecipitation, medicine.drug

Abstract

The present study reveals a link between protein arginine methyltransferase 5 (PRMT5) and Homebox A9 (HoxA9) in the regulation of cardiomyocyte hypertrophy. In cardiomyocyte hypertrophy induced by β-adrenergic receptor agonist isoprenaline (ISO), PRMT5 expression was decreased while HoxA9 was upregulated. Silencing of PRMT5 or inhibition of PRMT5 by its pharmacological inhibitor EPZ augmented the expressions of cardiomyocyte hypertrophic genes brain natriuretic peptide (BNP) and β-Myosin Heavy Chain (β-MHC), whereas overexpression of PRMT5 inhibited ISO-induced cardiomyocyte hypertrophy, suggesting that PRMT5 ameliorates cardiomyocyte hypertrophy. On the contrary, HoxA9 promoted cardiomyocyte hypertrophy, as implied by the gain-of-function and loss-of-function experiments. HoxA9 was involved in the regulation of PRMT5 in cardiomyocyte hypertrophy, since HoxA9 knockdown prevented si-RPMT5-induced cardiomyocyte hypertrophy, and HoxA9 expression impaired the anti-hypertrophic effect of PRMT5. Co-immunoprecipitation experiments revealed that there were physical interactions between PRMT5 and HoxA9. The symmetric dimethylation level of HoxA9 was decreased by ISO or EPZ treatment, suggesting that HoxA9 is methylated by PRMT5. Additionally, PRMT5 repressed the expression of HoxA9. Chromatin immunoprecipitation (ChIP) assay demonstrated that HoxA9 could bind to the promoter of BNP, and that this binding affinity was further enhanced by ISO or EPZ. In conclusion, this study suggests that PRMT5 symmetric dimethylates HoxA9 and represses HoxA9 expression, thus impairing its binding to BNP promoter and ultimately protecting against cardiomyocyte hypertrophy. These findings provide a novel insight of the mechanism underlying the cardiac protective effect of PRMT5, and suggest potential therapeutic strategies of PRMT5 activation or HoxA9 inhibition in treatment of cardiac hypertrophy.

Published

2020

20. MicroRNA-214 contributes to Ang II-induced cardiac hypertrophy by targeting SIRT3 to provoke mitochondrial malfunction

Author

Zhongbao Yue, Yuehuai Hu, Sidong Cai, Wen-jing Yu, Jiantao Ye, Jingyan Li, Peiqing Liu, Yanqing Ding, Bai Li, Jing Lu, Yuhong Zhang, and Panxia Wang

Subjects

0301 basic medicine, Male, SIRT3, Cardiomyopathy, Cardiomegaly, Article, Mitochondria, Heart, Muscle hypertrophy, Cell Line, Pathogenesis, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, 0302 clinical medicine, Sirtuin 3, medicine, Animals, Humans, Pharmacology (medical), Myocytes, Cardiac, miR-214, Pharmacology, Mice, Knockout, Gene knockdown, biology, business.industry, Angiotensin II, Myocardium, General Medicine, medicine.disease, Cell biology, Mice, Inbred C57BL, MicroRNAs, 030104 developmental biology, 030220 oncology & carcinogenesis, Sirtuin, biology.protein, business

Abstract

Reduction of expression and activity of sirtuin 3 (SIRT3) contributes to the pathogenesis of cardiomyopathy via inducing mitochondrial injury and energy metabolism disorder. However, development of effective ways and agents to modulate SIRT3 remains a big challenge. In this study we explored the upstream suppressor of SIRT3 in angiotensin II (Ang II)-induced cardiac hypertrophy in mice. We first found that SIRT3 deficiency exacerbated Ang II-induced cardiac hypertrophy, and resulted in the development of spontaneous heart failure. Since miRNAs play crucial roles in the pathogenesis of cardiac hypertrophy, we performed miRNA sequencing on myocardium tissues from Ang II-infused Sirt3 −/− and wild type mice, and identified microRNA- 214 (miR-214) was significantly up-regulated in Ang II-infused mice. Similar results were also obtained in Ang II-treated neonatal mouse cardiomyocytes (NMCMs). Using dual-luciferase reporter assay we demonstrated that SIRT3 was a direct target of miR-214. Overexpression of miR-214 in vitro and in vivo decreased the expression of SIRT3, which resulted in extensive mitochondrial damages, thereby facilitating the onset of hypertrophy. In contrast, knockdown of miR-214 counteracted Ang II-induced detrimental effects via restoring SIRT3, and ameliorated mitochondrial morphology and respiratory activity. Collectively, these results demonstrate that miR-214 participates in Ang II-induced cardiac hypertrophy by directly suppressing SIRT3, and subsequently leading to mitochondrial malfunction, suggesting the potential of miR-214 as a promising intervention target for antihypertrophic therapy.

Published

2020

21. Sorting nexin 3 induces heart failure via promoting retromer-dependent nuclear trafficking of STAT3

Author

Peiqing Liu, Xiaolei Zhang, Junjian Wang, Jing Lu, Mengya Liang, Yuqing Huo, Panxia Wang, Suowen Xu, Duanping Sun, Yuehuai Hu, Zhongkai Wu, and Zhuoming Li

Subjects

0301 basic medicine, Cardiac function curve, STAT3 Transcription Factor, Transgene, Proximity ligation assay, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Medicine, Animals, Humans, STAT3, Molecular Biology, Sorting Nexins, Cell Nucleus, Heart Failure, Mice, Knockout, Gene knockdown, biology, business.industry, Cell Biology, medicine.disease, Cell biology, Up-Regulation, Mice, Inbred C57BL, Sorting nexin, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, Heart failure, STAT protein, biology.protein, business, Signal Transduction

Abstract

Sorting nexins (SNXs), the retromer-associated cargo binding proteins, have emerged as critical regulators of the trafficking of proteins involved in the pathogenesis of diverse diseases. However, studies of SNXs in the development of cardiovascular diseases, especially cardiac hypertrophy and heart failure, are lacking. Here, we ask whether SNX3, the simplest structured isoform in the SNXs family, may act as a key inducer of myocardial injury. An increased level of SNX3 was observed in failing hearts from human patients and mice. Cardiac-specific Snx3 knockout (Snx3-cKO) mice and Snx3 transgenic (Snx3-cTg) mice were generated to evaluate the role of Snx3 in myocardial hypertrophy, fibrosis, and heart function by morphology, echocardiography, histological staining, and hypertrophic biomarkers. We report that Snx3-cKO in mice significantly protected against isoproterenol (ISO)-induced cardiac hypertrophy at 12 weeks. Conversely, Snx3-cTg mice were more susceptible to ISO-induced cardiac hypertrophy at 12 weeks and showed aggravated cardiac injury even heart failure at 24 weeks. Immunoprecipitation-based mass spectrometry, immunofluorescent staining, co-immunoprecipitation, localized surface plasmon resonance, and proximity ligation assay were performed to examine the direct interaction of SNX3-retromer with signal transducer and activator of transcription 3 (STAT3). We discovered that STAT3 was a new interacting partner of SNX3-retromer, and SNX3-retromer served as an essential platform for assembling gp130/JAK2/STAT3 complexes and subsequent phosphorylation of STAT3 by direct combination at EE. SNX3-retromer and STAT3 complexes were transiently imported into the nucleus after hypertrophic stimuli. The pharmacological inhibition or knockdown of STAT3 reversed SNX3 overexpression-induced myocardial injury. STAT3 overexpression blunts the beneficial function of SNX3 knockdown on hypertrophic cardiomyocytes. We show that SNX3-retromer promoted importin α3-mediated STAT3 nuclear trafficking and ultimately leading to cardiac injury. Taken together, our study reveals that SNX3 plays a key role in cardiac function and implicates SNX3 as a potential therapeutic target for cardiac hypertrophy and heart failure.

Published

2020

22. Sorting nexin 3 induces myocardial injury via promoting retromer-dependent nuclear trafficking of STAT3

Author

Peiqing Liu, Suowen Xu, Mengya Liang, Jing Lu, Zhuoming Li, Juanjian Wang, Yuehuai Hu, Yuqing Huo, Duanping Sun, Panxia Wang, Zhongkai Wu, and Xiaolei Zhang

Subjects

Sorting nexin, Retromer, biology, biology.protein, STAT3, Cell biology

Abstract

Sorting nexins (SNXs), the retromer-associated cargo binding proteins, have emerged as critical regulators of the trafficking of proteins involved in the pathogenesis of diverse diseases. However, studies of SNXs in the development of cardiovascular diseases, especially pathological cardiac hypertrophy, are lacking. Here, we asked whether SNX3, the simplest structured isoform in the SNXs family, may act as a key inducer of myocardial injury. We reported that increased level of SNX3 was observed in failing hearts from human patients and mice. Cardiac-specific Snx3 knockout (Snx3-cKO) in mice significantly protected against isoproterenol (ISO) -induced cardiac injury at 12 weeks. Conversely, cardiac-specific Snx3 transgenic (Snx3-cTg) mice were more susceptible to ISO-induced cardiac injury at 12 weeks, and showed aggravated cardiac injury even heart failure at 24 weeks. Immunoprecipitation-based mass spectrometry (IP-MS), immunofluorescent staining, co-immunoprecipitation and localized surface plasmon resonance (LSPR) were performed to examine the direct interaction of SNX3-retromer with STAT3. STAT3 was discovered as a new interacting partner of SNX3-retromer, and SNX3-retromer served as an essential platform for assembling gp130/JAK2/STAT3 complexes and subsequent phosphorylation of STAT3 by direct combination at early endosomes. SNX3-retromer and STAT3 complexes were transiently imported into the nucleus after hypertrophic stimuli. Moreover, SNX3-retromer promoted importin α3-mediated STAT3 nuclear trafficking and ultimately leading to cardiac injury. Also, pharmacological inhibition of STAT3 reversed SNX3 overexpression-induced myocardial injury in vivo and in vitro. Taken together, our study reveals that SNX3 plays a key role in cardiac function and implicates SNX3 as a potential therapeutic target for cardiac hypertrophy and heart failure.

Published

2020

23. Angiopoietin-2 induces angiogenesis via exosomes in human hepatocellular carcinoma

Author

Peiqing Liu, Wei-bang Yang, Jin-xing Wei, Li-Hong Lv, Jin-xin Duan, Qing-fang Han, Guolin Li, Jun Min, Shao-bin Wu, Panxia Wang, Jiyan Xie, and Wen-feng Zhuo

Subjects

0301 basic medicine, Carcinoma, Hepatocellular, Epithelial-Mesenchymal Transition, CRISPR-Cas systems, Hepatocellular carcinoma, Angiogenesis, lcsh:Medicine, Exosomes, Biochemistry, Exosome, Angiopoietin-2, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells, Humans, Recycling, Epithelial–mesenchymal transition, lcsh:QH573-671, Molecular Biology, Matrigel, Migration Assay, Neovascularization, Pathologic, biology, lcsh:Cytology, Chemistry, Research, lcsh:R, Liver Neoplasms, Cell Biology, Angiopoietin receptor, Endocytosis, Microvesicles, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, biology.protein

Abstract

Background Hepatocellular carcinoma (HCC) is the most common primary liver cancer and is a highly vascularized solid tumor. Angiopoietin-2 (ANGPT2) has been described as an attractive target for antiangiogenic therapy. Exosomes are small extracellular vesicles secreted by most cell types and contribute to cell-to-cell communication by delivering functional cargo to recipient cells. The expression of ANGPT2 in tumor-derived exosomes remains unknown. Methods We detected the ANGPT2 expression in HCC-derived exosomes by immunoblotting, enzyme-linked immunosorbent assay and immunogold labeling, then observed exosomal ANGPT2 internalization and recycling by confocal laser scanning microscopy, co-immunoprecipitation and immunoblotting. We used two HCC cell lines (Hep3B and MHCC97H) to overexpress ANGPT2 by lentivirus infection or knockdown ANGPT2 by the CRISPR/Cas system, then isolated exosomes to coculture with human umbilical vein endothelial cells (HUVECs) and observed the angiogenesis by Matrigel microtubule formation assay, transwell migration assay, wound healing assay, cell counting kit-8 assay, immunoblotting and in vivo tumorigenesis assay. Results We found that HCC-derived exosomes carried ANGPT2 and delivered it into HUVECs by exosome endocytosis, this delivery led to a notable increase in angiogenesis by a Tie2-independent pathway. Concomitantly, we observed that HCC cell-secreted exosomal ANGPT2 was recycled by recipient HUVECs and might be reused. In addition, the CRISPR-Cas systems to knock down ANGPT2 significantly inhibited the angiogenesis induced by HCC cell-secreted exosomal ANGPT2, and obviously suppressed the epithelial-mesenchymal transition activation in HCC. Conclusions Taken together, these results reveal a novel pathway of tumor angiogenesis induced by HCC cell-secreted exosomal ANGPT2 that is different from the classic ANGPT2/Tie2 pathway. This way may be a potential therapeutic target for antiangiogenic therapy.

Published

2020

24. PARP1 interacts with HMGB1 and promotes its nuclear export in pathological myocardial hypertrophy

Author

Qian Li, Hanwei Yang, Shuya Sun, Jiantao Ye, Panxia Wang, Peiqing Liu, Zhuoming Li, Zhen Guo, Luping Wang, and Jing Lu

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Cell, Active Transport, Cell Nucleus, Poly (ADP-Ribose) Polymerase-1, Cardiomegaly, chemical and pharmacologic phenomena, Chromosomal translocation, HMGB1, Article, Rats, Sprague-Dawley, Phenylephrine, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Animals, Myocytes, Cardiac, Pharmacology (medical), Secretion, HMGB1 Protein, Nuclear export signal, Cell Nucleus, Pharmacology, biology, Chemistry, Angiotensin II, Isoproterenol, General Medicine, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Cytoplasm, 030220 oncology & carcinogenesis, biology.protein, medicine.drug

Abstract

High-mobility group box 1 (HMGB1) exhibits various functions according to its subcellular location, which is finely conditioned by diverse post-translational modifications, such as acetylation. The nuclear HMGB1 may prevent from cardiac hypertrophy, whereas its exogenous protein is proven to induce hypertrophic response. This present study sought to investigate the regulatory relationships between poly(ADP-ribose) polymerase 1 (PARP1) and HMGB1 in the process of pathological myocardial hypertrophy. Primary-cultured neonatal rat cardiomyocytes (NRCMs) were respectively incubated with three cardiac hypertrophic stimulants, including angiotensin II (Ang II), phenylephrine (PE), and isoproterenol (ISO), and cell surface area and the mRNA expression of hypertrophic biomarkers were measured. the catalytic activity of PARP1 was remarkably enhanced, meanwhile HMGB1 excluded from the nucleus. PARP1 overexpression by infecting with adenovirus PARP1 (Ad-PARP1) promoted the nuclear export of HMGB1, facilitated its secretion outside the cell, aggravated cardiomyocyte hypertrophy, which could be alleviated by HMGB1 overexpression. PE treatment led to the similar results, while that effect was widely depressed by PARP1 silencing or its specific inhibitor AG14361. Moreover, SD rats were intraperitoneally injected with 3-aminobenzamide (3AB, 20 mg/kg every day, a well-established PARP1 inhibitor) 7 days after abdominal aortic constriction (AAC) surgery for 6 weeks, echocardiography and morphometry of the hearts were measured. Pre-treatment of 3AB relieved AAC-caused the translocation of nuclear HMGB1 protein, cardiac hypertrophy, and heart dysfunction. Our research offers a novel evidence that PARP1 combines with HMGB1 and accelerates its translocation from nucleus to cytoplasm, and the course finally causes cardiac hypertrophy.

Published

2018

25. SIRT3 prevents angiotensin II-induced renal tubular epithelial-mesenchymal transition by ameliorating oxidative stress and mitochondrial dysfunction

Author

Shaorui Chen, Peiqing Liu, Ping He, Yi Huang, Hui Gao, Liying Liang, Wenwei Luo, Panxia Wang, Guo-shuai Feng, Zhongbao Yue, Zhuoming Li, and Huiqi Hong

Subjects

0301 basic medicine, Epithelial-Mesenchymal Transition, SIRT3, Systole, Down-Regulation, Blood Pressure, Biology, medicine.disease_cause, Biochemistry, Cell Line, 03 medical and health sciences, Endocrinology, Downregulation and upregulation, Superoxides, Sirtuin 3, Renin–angiotensin system, medicine, Animals, Epithelial–mesenchymal transition, Molecular Biology, Membrane Potential, Mitochondrial, Mice, Knockout, Kidney, Superoxide Dismutase, Angiotensin II, Mitochondria, Rats, Oxidative Stress, Kidney Tubules, 030104 developmental biology, medicine.anatomical_structure, Cytoprotection, embryonic structures, Tubulointerstitial fibrosis, Cancer research, Oxidative stress

Abstract

Silent mating type information regulation 2 homolog 3 (SIRT3) is a major protective mediator that ameliorates oxidative stress and mitochondrial dysfunction, which are associated with the pathogenesis of epithelial-mesenchymal transition (EMT). The present study was aimed to investigate the potential role of SIRT3 in renal tubular EMT both in vitro and in vivo. Firstly, we showed that the expression of SIRT3 was repressed in angiotensin II-induced EMT. SIRT3 deficiency triggered EMT response, while over-expression of SIRT3 attenuated EMT response. In addition, over-expression of SIRT3 repressed AngⅡ-induced excessive production of mitochondrial superoxide, as well as mitochondrial dysfunction evidenced by the maintenance of mitochondrial number and morphology, and the stabilization of mitochondrial membrane potential. In conclusion, these findings identify a protective role of SIRT3 against angiotensin II-induced EMT in the kidney, and suggest SIRT3 upregulation is a potential therapeutic strategy for the treatment of renal tubulointerstitial fibrosis.

Published

2018

26. C33(S), a novel PDE9A inhibitor, protects against rat cardiac hypertrophy through upregulating cGMP signaling

Author

Peiqing Liu, Jingyan Li, Yi Huang, Zhuoming Li, Guo-shuai Feng, Panxia Wang, Sidong Cai, Shaorui Chen, Hai-Bin Luo, and Ping He

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Cardiac output, Cardiomegaly, 030204 cardiovascular system & hematology, Rats, Sprague-Dawley, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, In vivo, Internal medicine, medicine, Animals, Myocyte, Myocytes, Cardiac, Pharmacology (medical), Enzyme Inhibitors, Cyclic GMP, Cells, Cultured, Pharmacology, Fetus, Ejection fraction, Dose-Response Relationship, Drug, business.industry, General Medicine, medicine.disease, Rats, Up-Regulation, Phospholamban, Dose–response relationship, Pyrimidines, 030104 developmental biology, Endocrinology, 3',5'-Cyclic-AMP Phosphodiesterases, Heart failure, Pyrazoles, Original Article, business, Signal Transduction

Abstract

Phosphodiesterase-9A (PDE9A) expression is upregulated during cardiac hypertrophy and heart failure. Accumulating evidence suggests that PDE9A might be a promising therapeutic target for heart diseases. The present study sought to investigate the effects and underlying mechanisms of C33(S), a novel selective PDE9A inhibitor, on cardiac hypertrophy in vitro and in vivo. Treatment of neonatal rat cardiomyocytes (NRCMs) with PE (100 μmol/L) or ISO (1 μmol/L) induced cardiac hypertrophy characterized by significantly increased cell surface areas and increased expression of fetal genes (ANF and BNP). Furthermore, PE or ISO significantly increased the expression of PDE9A in the cells; whereas knockdown of PDE9A significantly alleviated PE-induced hypertrophic responses. Moreover, pretreatment with PDE9A inhibitor C33(S) (50 and 500 nmol/L) or PF-7943 (2 μmol/L) also alleviated the cardiac hypertrophic responses in PE-treated NRCMs. Abdominal aortic constriction (AAC)-induced cardiac hypertrophy and ISO-induced heart failure were established in SD rats. In ISO-treated rats, oral administration of C33(S) (9, 3, and 1 mg·kg−1·d−1, for 3 consecutive weeks) significantly increased fractional shortening (43.55%±3.98%, 54.79%±1.95%, 43.98%±7.96% vs 32.18%±6.28%), ejection fraction (72.97%±4.64%, 84.29%±1.56%, 73.41%±9.37% vs 49.17%±4.20%) and cardiac output (60.01±9.11, 69.40±11.63, 58.08±8.47 mL/min vs 48.97±2.11 mL/min) but decreased the left ventricular internal diameter, suggesting that the transition to heart failure was postponed by C33(S). We further revealed that C33(S) significantly elevated intracellular cGMP levels, phosphorylation of phospholamban (PLB) and expression of SERCA2a in PE-treated NRCMs in vitro and in ISO-induced heart failure model in vivo. Our results demonstrate that C33(S) effectively protects against cardiac hypertrophy and postpones the transition to heart failure, suggesting that it is a promising agent in the treatment of cardiac diseases.

Published

2017

27. Synthesis of the novel PARP-1 inhibitor AG-690/11026014 and its protective effects on angiotensin II-induced mouse cardiac remodeling

Author

Shaorui Chen, Yi Huang, Guo-shuai Feng, Panxia Wang, Peiqing Liu, Ping He, Lan-Lan Lou, Min Liu, Cui-Ge Zhu, and Zhuoming Li

Subjects

Male, 0301 basic medicine, Cardiac function curve, medicine.medical_specialty, Cardiotonic Agents, Cardiac fibrosis, Poly (ADP-Ribose) Polymerase-1, Cardiomegaly, 03 medical and health sciences, Sirtuin 1, Western blot, In vivo, Internal medicine, medicine, Animals, Myocyte, Myocytes, Cardiac, Pharmacology (medical), Pharmacology, Ejection fraction, Ventricular Remodeling, medicine.diagnostic_test, business.industry, Angiotensin II, General Medicine, medicine.disease, Fibrosis, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Thioglycolates, Xanthines, cardiovascular system, Original Article, NAD+ kinase, business

Abstract

We previously identified AG-690/11026014 (6014) as a novel poly(ADP-ribose) polymerase-1 (PARP-1) inhibitor that effectively prevented angiotensin II (Ang II)-induced cardiomyocyte hypertrophy. In the present study, we reported a new synthesis route for 6014, and investigated its protective effects on Ang II-induced cardiac remodeling and cardiac dysfunction and the underlying mechanisms in mice. We designed a new synthesis route to obtain a sufficient quantity of 6014 for this in vivo study. C57BL/6J mice were infused with Ang II and treated with 6014 (10, 30, 90 mg·kg−1·d−1, ig) for 4 weeks. Then two-dimensional echocardiography was performed to assess the cardiac function and structure. Histological changes of the hearts were examined with HE staining and Masson's trichrome staining. The protein expression was evaluated by Western blot, immunohistochemistry and immunofluorescence assays. The activities of sirtuin-1 (SIRT-1) and the content of NAD+ were detected with the corresponding test kits. Treatment with 6014 dose-dependently improved cardiac function, including LVEF, CO and SV and reversed the changes of cardiac structure in Ang II-infused mice: it significantly ameliorated Ang II-induced cardiac hypertrophy evidenced by attenuating the enlargement of cardiomyocytes, decreased HW/BW and LVW/BW, and decreased expression of hypertrophic markers ANF, BNP and β-MHC; it also prevented Ang II-induced cardiac fibrosis, as implied by the decrease in excess accumulation of extracellular matrix (ECM) components collagen I, collagen III and FN. Further studies revealed that treatment with 6014 did not affect the expression levels of PARP-1, but dose-dependently inhibited the activity of PARP-1 and subsequently restored the activity of SIRT-1 in heart tissues due to the decreased consumption of NAD+ and attenuated Poly-ADP-ribosylation (PARylation) of SIRT-1. In conclusion, the novel PARP-1 inhibitor 6014 effectively protects mice against AngII-induced cardiac remodeling and improves cardiac function. Thus, 6014 might be a potential therapeutic agent for heart diseases..

Published

2017

28. Histone H4R3 symmetric di-methylation by Prmt5 protects against cardiac hypertrophy via regulation of Filip1L/β-catenin

Author

Zhuoming Li, Peiqing Liu, Panxia Wang, Sidong Cai, Tingting Xie, Yanqing Ding, Junjian Wang, Zhenzhen Li, Jiantao Ye, Jingyan Li, Rui Lan, and Jing Lu

Subjects

0301 basic medicine, Male, Protein-Arginine N-Methyltransferases, Histone lysine methylation, Arginine, Methylation, Ventricular Function, Left, Muscle hypertrophy, Epigenesis, Genetic, Histones, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Histone arginine methylation, Animals, Myocytes, Cardiac, Epigenetics, Cells, Cultured, beta Catenin, Pharmacology, biology, Ventricular Remodeling, Chemistry, Protein arginine methyltransferase 5, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Histone, 030220 oncology & carcinogenesis, biology.protein, Hypertrophy, Left Ventricular, Signal Transduction

Abstract

Background and purpose Although histone lysine methylation has been extensively studied for their participation in pathological cardiac hypertrophy, the potential regulatory role of histone arginine methylation remains to be elucidated. The present study focused on H4R3 symmetric di-methylation (H4R3me2s) induced by protein arginine methyltransferase 5 (Prmt5), and explored its epigenetic regulation and underlying mechanisms in cardiomyocyte hypertrophy. Methods and results 1. The expressions of Prmt5 and H4R3me2s were suppressed in cardiac hypertrophy models in vivo and in vitro; 2. Prmt5 silencing or its inhibitor EPZ, or knockdown of cooperator of Prmt5 (Copr5) to disrupt H4R3me2s, facilitated cardiomyocyte hypertrophy, whereas overexpression of wild type Prmt5 rather than the inactive mutant protected cardiomyocytes against hypertrophy; 3. ChIP-sequence analysis identified Filip1L as a target gene of Prmt5-induced H4R3me2s; 4. Knockdown or inhibition of Prmt5 impaired Filip1L transcription and subsequently prevented β-catenin degradation, thus augmenting cardiomyocyte hypertrophy. Conclusions The present study reveals that Prmt5-induced H4R3me2s ameliorates cardiomyocyte hypertrophy by transcriptional upregulation of Filip1L and subsequent enhancement of β-catenin degradation. Deficiency of Prmt5 and the resulting suppression of H4R3me2s might facilitate the development of pathological cardiac hypertrophy. Prmt5 might serve as a key epigenetic regulator in pathological cardiac hypertrophy.

Published

2019

29. PKCζ interacts with STAT3 and promotes its activation in cardiomyocyte hypertrophy

Author

Peiqing Liu, Xiaoying Zhang, Hui Gao, Sidong Cai, Jia You, Peiye Shen, Yi Huang, Wenwei Luo, Junying Huang, Zhuoming Li, Panxia Wang, and Jingyan Li

Subjects

STAT3 Transcription Factor, 0301 basic medicine, medicine.medical_specialty, Green Fluorescent Proteins, Cell, Cardiomegaly, 030204 cardiovascular system & hematology, Rats, Sprague-Dawley, STAT3, Phenylephrine, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Animals, Medicine, Gene silencing, Myocytes, Cardiac, RNA, Small Interfering, Phosphorylation, Cells, Cultured, Protein Kinase C, Protein kinase C, PKCζ, Pharmacology, Gene knockdown, biology, business.industry, lcsh:RM1-950, Rats, Cell biology, Cardiac hypertrophy, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, biology.protein, STAT protein, Molecular Medicine, Signal transduction, business, Plasmids

Abstract

This study was aimed to investigate the crosstalk between protein kinase C ζ (PKCζ) and signal transducer and activator of transcription 3 (STAT3) in cardiomyocyte hypertrophy. In neonatal rat cardiomyocyte hypertrophic model induced by phenylephrine (PE), the levels of phosphorylated PKCζ and phosphorylated STAT3 were significantly increased, suggesting the activation of both PKCζ and STAT3 in cardiomyocyte hypertrophy. Overexpression of PKCζ by adenovirus infection elevated the expressions of hypertrophic markers atrial natriuretic factor (ANF) and brains natriuretic polypeptide (BNP), as well as the cell surface area; while genetic silencing of PKCζ inhibited PE-induced cardiomyocyte hypertrophy. An interaction between PKCζ and STAT3 in cardiomyocytes was shown by co-immunoprecipitation experiments. Overexpression of PKCζ increased the phosphorylated level of STAT3 at both Ser727 and Tyr705, promoted the nuclear translocation of STAT3, and enhanced the expression of STAT3 downstream target genes c-fos and angiotensinogen (aGT); whereas PKCζ knockdown prevented PE-induced STAT3 activation, nuclear shuttling and transcriptional activation. In conclusion, PKCζ interacts with STAT3 and promotes its activation in cardiomyocyte hypertrophy. Strategies targeting inhibition of PKCζ-STAT3 signaling pathway suggest a therapeutic potential for cardiac hypertrophy.

Published

2016

30. Electrochemical biosensor based on gold nanoflowers-encapsulated magnetic metal-organic framework nanozymes for drug evaluation with in-situ monitoring of H2O2 released from H9C2 cardiac cells

Author

Panxia Wang, Yuehuai Hu, Peiqing Liu, Jing Lu, Zuanguang Chen, and Duanping Sun

Subjects

Detection limit, Materials science, Nanocomposite, Metals and Alloys, Nanotechnology, 02 engineering and technology, Electrolyte, 010402 general chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, 01 natural sciences, 0104 chemical sciences, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Catalysis, Nanomaterials, chemistry.chemical_compound, chemistry, Electrode, Materials Chemistry, Electrical and Electronic Engineering, 0210 nano-technology, Instrumentation, Molybdenum disulfide, Biosensor

Abstract

A novel electrochemical biosensor was fabricated for the determination of hydrogen peroxide (H2O2) by electrodeposition of gold nanoflowers (AuNFs) on molybdenum disulfide (MoS2) nanosheets-supported magnetic metal-organic framework (MMOF) Fe3O4@ZIF-8 hybrid nanozymes. Fe3O4@ZIF-8 nanomaterial was selected on account of the high peroxidase-mimicking activity of magnetic Fe3O4 nanoparticle and the large pore size and surface area of metal-organic framework ZIF-8. However, we found that the MMOF Fe3O4@ZIF-8 nanomaterial was easily dissoluted into the electrolyte solution followed by an unreproducible electrochemical response. MoS2 nanosheets and one-step electrodeposition of gold nanostructures can largely enhance the long-term stability, conductivity and catalytic performance. With the help of MoS2 nanosheets and electrodeposited gold thin layer, it can have an important impact on the retaining of surface states of Fe3O4@ZIF-8 nanomaterials to keep the electrocatalytic activity. The obtained hybrid nanocomposites (AuNFs/Fe3O4@ZIF-8-MoS2) exhibited prominent electrocatalytic activity for the reduction of H2O2 and the fabricated biosensor detected H2O2 with a low detection limit of 0.9 μM and an ultra-wide linear detection range of 5 μM–120 mM. Moreover, this electrochemical biosensor was successfully performed to detect H2O2 concentration released from H9C2 cardiac cells under drug stimulation. These results indicated that this modified electrode can serve as a general and powerful platform to detect other disease biomarkers for drug evaluation.

Published

2020

31. Dkk1 exacerbates doxorubicin-induced cardiotoxicity by inhibiting Wnt/β-catenin signaling pathway

Author

Zhen Guo, Hong Li, Peiqing Liu, Liying Liang, Panxia Wang, Qianqian Wang, Kaiteng Guo, Rui Lan, Yalin Tu, and Jing Lu

Subjects

Male, musculoskeletal diseases, Cardiomyopathy, Apoptosis, Mitochondrion, Biology, Cell Line, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, In vivo, polycyclic compounds, medicine, Animals, Doxorubicin, Wnt Signaling Pathway, beta Catenin, 030304 developmental biology, 0303 health sciences, Cardiotoxicity, Antibiotics, Antineoplastic, organic chemicals, technology, industry, and agriculture, Wnt signaling pathway, Cell Biology, medicine.disease, Rats, Up-Regulation, Wnt Proteins, carbohydrates (lipids), DKK1, Cancer research, Intercellular Signaling Peptides and Proteins, 030217 neurology & neurosurgery, medicine.drug

Abstract

The cancer clinical therapy of Doxorubicin (Dox) is limited by its life-threatening cardiotoxic effects. Dickkopf-1 (Dkk1), the founding member of Dkk family, is best studied and functions as an antagonist of canonical Wnt/β-catenin. Dkk1 is considered to play a broad role in a variety of biological processes, but its effects on Dox-induced cardiomyopathy is poorly understood. Here, we found that Dkk1 was significantly increased in Dox-treated groups, and this increase exacerbated Dox-induced cardiomyocyte apoptosis and mitochondrial dysfunction. Overexpressing Dkk1 aggravated Dox-induced cardiotoxicity in H9C2 cells. Similar results were detected when adding the Dkk1 active protein extracellularly. Conversely, specific antibody blocking extracellular Dkk1 attenuated Dox-cardiotoxic response. Adenovirus encoding Dkk1 was transduced through intramyocardial injection and exacerbated Dox-induced cardiomyocyte apoptosis, mitochondrial damage and heart injury in vivo. Furthermore, Wnt/β-catenin signaling was inhibited in Dox-induced cardiotoxicity, the re-activation of β-catenin relieved overexpressed Dkk1 or Dox-induced cardiotoxicity. In conclusion, these results uncovered that the crucial role of Dkk1-Wnt/β-catenin signaling axis in the process of Dox-induced cardiotoxicity and provided novel insights into the potential mechanism on cardiomyopathy caused by clinical application of Dox.

Published

2019

32. Sirtuin 1 represses PKC‐ζ activity through regulating interplay of acetylation and phosphorylation in cardiac hypertrophy

Author

Zhen Guo, Yuehuai Hu, Peiqing Liu, Luping Wang, Zhenzhen Li, Zhuoming Li, Jingyan Li, Xiaolei Zhang, Sidong Cai, Panxia Wang, Wenwei Luo, Jing Lu, Minghui Wang, Kaiteng Guo, Junying Huang, and Hui Gao

Subjects

Male, 0301 basic medicine, Ceramide, Cardiomegaly, Muscle hypertrophy, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Sirtuin 1, Animals, Myocyte, Phosphatidylinositol, Phosphorylation, Protein Kinase C, Protein kinase C, Pharmacology, biology, Kinase, Acetylation, Research Papers, Rats, Cell biology, 030104 developmental biology, chemistry, biology.protein

Abstract

Background and purpose Activation of PKC-ζ is closely linked to the pathogenesis of cardiac hypertrophy. PKC-ζ can be activated by certain lipid metabolites such as phosphatidylinositol (3,4,5)-trisphosphate and ceramide. However, its endogenous negative regulators are not well defined. Here, the role of the sirtuin1-PKC-ζ signalling axis and the underlying molecular mechanisms were investigated in cardiac hypertrophy. Experimental approach Cellular hypertrophy in cultures of cardiac myocytes, from neonatal Sprague-Dawley rats, was monitored by measuring cell surface area and the mRNA levels of hypertrophic biomarkers. Interaction between sirtuin1 and PKC-ζ was investigated by co-immunoprecipitation and confocal immunofluorescence microscopy. Sirtuin1 activation was enhanced by resveratrol treatment or Ad-sirtuin1 transfection. A model of cardiac hypertrophy in Sprague-Dawley rats was established by abdominal aortic constriction surgery or induced by isoprenaline in vivo. Key results Overexpression of PKC-ζ led to cardiac hypertrophy and increased activity of NF-κB, ERK1/2 and ERK5, which was ameliorated by sirtuin1 overexpression. Enhancement of sirtuin1 activity suppressed acetylation of PKC-ζ, hindered its binding to phosphoinositide-dependent kinase 1 and inhibited PKC-ζ phosphorylation in cardiac hypertrophy. Consequently, the downstream pathways of PKC-ζ' were suppressed in cardiac hypertrophy. This regulation loop suggests a new role for sirtuin1 in mediation of cardiac hypertrophy. Conclusions and implications Sirtuin1 is an endogenous negative regulator for PKC-ζ and mediates its activity via regulating the acetylation and phosphorylation in the pathogenesis of cardiac hypertrophy. Targeting the sirtuin1-PKC-ζ signalling axis may suggest a novel therapeutic approach against cardiac hypertrophy.

Published

2018

33. sFRP1 has a biphasic effect on doxorubicin-induced cardiotoxicity in a cellular location-dependent manner in NRCMs and Rats

Author

Jingyan Li, Shuya Sun, Peiqing Liu, Jing Lu, Junjian Wang, Yuehuai Hu, Kaiteng Guo, Yiqiang Zhang, Panxia Wang, Zhen Guo, Qiyao Zheng, and Jianmin Jiang

Subjects

0301 basic medicine, Male, Health, Toxicology and Mutagenesis, Poly (ADP-Ribose) Polymerase-1, Apoptosis, Ataxia Telangiectasia Mutated Proteins, 010501 environmental sciences, Pharmacology, Toxicology, 01 natural sciences, Rats, Sprague-Dawley, 03 medical and health sciences, PARP1, In vivo, polycyclic compounds, medicine, Animals, Humans, Doxorubicin, Secretion, Wnt Signaling Pathway, beta Catenin, 0105 earth and related environmental sciences, Cardiotoxicity, Gene knockdown, Antibiotics, Antineoplastic, Chemistry, Membrane Proteins, General Medicine, In vitro, carbohydrates (lipids), 030104 developmental biology, Case-Control Studies, Intercellular Signaling Peptides and Proteins, Intracellular, medicine.drug

Abstract

Doxorubicin (Dox) is an effective anticancer drug, however, its clinical application is restricted by the life-threatening cardiotoxic effects. Secreted Frizzled-related protein 1 (sFRP1) has been reported to participate in both the cancer and cardiovascular diseases and was one of the differential expression genes in normal hearts compared with Dox-treated hearts. Thus, it is important to reveal the potential role of sFRP1 in Dox-induced cardiotoxicity. Here, we show that sFRP1 has a biphasic effect on Dox-induced cardiotoxicity in a location-dependent manner. The secretion of sFRP1 was significantly increased in Dox-treated neonatal rat cardiomyocytes (NRCMs) (1 µM) and SD rats (5 mg/kg/injection at day 1, 5, and 9, i.p.). Adding the anti-sFRP1 antibody (0.5 µg/ml) and inhibiting sFRP1 secretion by caffeine (5 mM) both relieved Dox-induced cardiotoxicity through activating Wnt/β-catenin signaling, whereas increasing the secretion of sFRP1 by heparin (100 µg/ml) had the opposite effect. The intracellular level of sFRP1 was significantly decreased after Dox treatment both in vitro and in vivo. Knockdown of sFRP1 by sgRNA aggravated Dox-induced cardiotoxicity, while moderate overexpression of sFRP1 by Ad-sFRP1 exhibited protective effect. Besides, poly(ADP-ribosyl) polymerase-1 (PARP1) was screened as an interacting partner of sFRP1 in NRCMs by mass spectrometry. Our results suggested that the intracellular sFRP1 protected NRCMs from Dox-induced cardiotoxicity by interacting with PARP1. Thus, our results provide a novel evidence that sFRP1 has a biphasic effect on Dox-induced cardiotoxicity. In addition, the oversecretion of sFRP1 might be used as a biomarker to indicate the occurrence of cardiotoxicity induced by Dox treatment.

Published

2018

34. Chrysophanol protects against doxorubicin-induced cardiotoxicity by suppressing cellular PARylation

Author

Jingyan Li, Yuehuai Hu, Junjian Wang, Jing Lu, Si Gao, Dayue Darrel Duan, Kaiteng Guo, Peiqing Liu, Panxia Wang, Zhen Guo, Jianmin Jiang, and Duanping Sun

Subjects

IVSd, end-diastolic interventricular septum, Cardiomyopathy, Apoptosis, Pharmacology, Mitochondrion, NS, normal saline, 0302 clinical medicine, PARP1, LVPWd, LV end-diastolic posterior wall thickness, LVIDs, LV end-systolic internal diameter, polycyclic compounds, General Pharmacology, Toxicology and Pharmaceutics, LVIDd, LV end-diastolic internal diameter, Cardioprotection, 0303 health sciences, FS, fractional shortening, HR, heart rate, PARylation, poly(ADP-ribosyl)ation, Chemistry, ANOVA, one-way analysis of variance, Mitochondria, LVEDV, LV end-diastolic volume, 030220 oncology & carcinogenesis, RCR, respiratory control ratio, PAR, polymers of ADP-ribose, medicine.drug, Original article, CO, cardiac output, 3AB, 3-aminobenzamide, PBS, phosphate-buffered saline, LVPWs, LV end-systolic posterior wall thickness, PARP1, poly(ADP-ribose) polymerase 1, Cyt c, Cytochrome c, IVSs, end-systolic interventricular septum, CMC-Na, sodium carboxymethyl, PARylated, poly(ADP-ribosyl)ated, 03 medical and health sciences, ROS, reactive oxygen species, FBS, fetal bovine serum, HE, hematoxylin-eosin, medicine, LV, end-systolic volume, EF, ejection fraction, Doxorubicin, 030304 developmental biology, Cardiotoxicity, Rh123, rhodamine 123, lcsh:RM1-950, ADR, adriamycin, TUNEL, TdT-mediated dUTP nick end labeling, medicine.disease, DOX, doxorubicin, carbohydrates (lipids), PARylation, lcsh:Therapeutics. Pharmacology, Chrysophanol, SD, Sprague–Dawley, Ectopic expression, CHR, chrysophanol, VDAC1, voltage dependent anion channel 1

Abstract

The clinical application of doxorubicin (DOX) in cancer chemotherapy is limited by its life-threatening cardiotoxic effects. Chrysophanol (CHR), an anthraquinone compound isolated from the rhizome of Rheum palmatum L., is considered to play a broad role in a variety of biological processes. However, the effects of CHR׳s cardioprotection in DOX-induced cardiomyopathy is poorly understood. In this study, we found that the cardiac apoptosis, mitochondrial injury and cellular PARylation levels were significantly increased in H9C2 cells treated by Dox, while these effects were suppressed by CHR. Similar results were observed when PARP1 activity was suppressed by its inhibitors 3-aminobenzamide (3AB) and ABT888. Ectopic expression of PARP1 effectively blocked this CHR׳s cardioprotection against DOX-induced cardiomyocyte injury in H9C2 cells. Furthermore, pre-administration with both CHR and 3AB relieved DOX-induced cardiac apoptosis, mitochondrial impairment and heart dysfunction in Sprague–Dawley rat model. These results revealed that CHR protects against DOX-induced cardiotoxicity by suppressing cellular PARylation and provided critical evidence that PARylation may be a novel target for DOX-induced cardiomyopathy., Graphical abstract CHR protected against doxorubicin (DOX)-induced cardiomyocytes apoptosis, mitochondrial injury and heart dysfunction by suppressing cellular PARylation in vitro and in vivo.fx1, Highlights • CHR protected against DOX-induced apoptosis, mitochondrial injury and heart dysfunction in vivo and in vitro. • PARP1 inhibition significantly suppressed DOX-induced cardiomyocyte injury. • Ectopic expression of PARP1 blocked the CHR’s cardioprotection.

Published

2018

35. Protocatechuic aldehyde protects against isoproterenol-induced cardiac hypertrophy via inhibition of the JAK2/STAT3 signaling pathway

Author

Yuhong Zhang, Peiqing Liu, Jing Lu, Panxia Wang, Xiu-li Fang, Jing Yuan, Huiqi Hong, Yajun Liu, and Jiantao Ye

Subjects

0301 basic medicine, Male, STAT3 Transcription Factor, medicine.medical_specialty, Cardiotonic Agents, Catechols, Inflammation, Cardiomegaly, 030204 cardiovascular system & hematology, medicine.disease_cause, Salvia miltiorrhiza, Muscle hypertrophy, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, Internal medicine, medicine, Animals, Myocytes, Cardiac, STAT3, Cells, Cultured, Pharmacology, biology, Chemistry, Isoproterenol, General Medicine, Janus Kinase 2, 030104 developmental biology, Endocrinology, Benzaldehydes, biology.protein, Protocatechuic aldehyde, medicine.symptom, Signal transduction, Oxidative stress, Signal Transduction

Abstract

Protocatechuic aldehyde (PCA) is a natural compound found in the Chinese herb Salvia miltiorrhiza. It has been shown to possess multiple biological activities and to protect the cardiovascular system against oxidative stress, inflammation, and atherosclerosis. However, the potential effects of PCA on cardiac hypertrophy remain to be investigated. In this study, we showed that isoproterenol treatment (ISO, 10 μM for 24 h) induced significant hypertrophy in cultured neonatal rat cardiomyocytes, as manifested by enlargement of cell surface area (1.74-fold greater than that of the control, p

Published

2018

36. JMJD3 inhibition protects against isoproterenol-induced cardiac hypertrophy by suppressing β-MHC expression

Author

Zhen Guo, Zhenzhen Li, Junjian Wang, Jiantao Ye, Jingyan Li, Jing Lu, Yao Zhong, Peiqing Liu, Panxia Wang, and Kaiteng Guo

Subjects

0301 basic medicine, Cell physiology, Male, Jumonji Domain-Containing Histone Demethylases, Regulator, Cardiomegaly, Biochemistry, Methylation, Muscle hypertrophy, Histones, Rats, Sprague-Dawley, 03 medical and health sciences, Endocrinology, In vivo, Gene silencing, Animals, Myocytes, Cardiac, Epigenetics, Promoter Regions, Genetic, Molecular Biology, biology, Myosin Heavy Chains, Chemistry, Lysine, Isoproterenol, Benzazepines, Cell biology, Demethylation, Up-Regulation, Mice, Inbred C57BL, 030104 developmental biology, Histone, Pyrimidines, Animals, Newborn, Gene Knockdown Techniques, biology.protein, Demethylase

Abstract

Jumonji domain-containing protein D3 (JMJD3), a histone 3 lysine 27 (H3K27) demethylase, has been extensively studied for their participation in development, cellular physiology and a variety of diseases. However, its potential roles in cardiovascular system remain unknown. In this study, we found that JMJD3 played a pivotal role in the process of cardiac hypertrophy. JMJD3 expression was elevated by isoproterenol (ISO) stimuli both in vitro and in vivo. Overexpression of wild-type JMJD3, but not the demethylase-defective mutant, promoted cardiomyocyte hypertrophy, as implied by increased cardiomyocyte surface area and the expression of hypertrophy marker genes. In contrary, JMJD3 silencing or its inhibitor GSK-J4 suppressed ISO-induced cardiac hypertrophy. Mechanistically, JMJD3 was recruited to demethylate H3K27me3 at the promoter of β-MHC to promote its expression and cardiac hypertrophy. Thus, our results reveal that JMJD3 may be a key epigenetic regulator of β-MHC expression in cardiomyocytes and a potential therapeutic target for cardiac hypertrophy.

Published

2018

37. PARP1 interacts with STAT3 and retains active phosphorylated-STAT3 in nucleus during pathological myocardial hypertrophy

Author

Luping Wang, Hanwei Yang, Panxia Wang, Peiqing Liu, Zhuoming Li, Qian Li, Yinzi Tan, and Jing Lu

Subjects

0301 basic medicine, Male, STAT3 Transcription Factor, Transcription, Genetic, Poly (ADP-Ribose) Polymerase-1, Cardiomegaly, Biochemistry, Rats, Sprague-Dawley, 03 medical and health sciences, Phenylephrine, 0302 clinical medicine, Endocrinology, PARP1, medicine, Extracellular, Pressure, Animals, Myocytes, Cardiac, Phosphorylation, STAT3, Molecular Biology, Polymerase, Cell Nucleus, Gene knockdown, biology, Chemistry, Myocardium, Janus Kinase 2, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, 030220 oncology & carcinogenesis, STAT protein, biology.protein, Nucleus, Protein Binding

Abstract

The activation of signal transducer and activator of transcription 3 (STAT3) positively regulates myocardial hypertrophy, and its transcriptional activity is finely conditioned by diverse extracellular growth factors and cytokines. Here, we introduce novel evidence that poly(ADP-ribose) polymerase 1 (PARP1) interacts with STAT3 and promotes its activation in cardiomyocytes and rat heart tissues. PARP1 activity and phosphorylated STAT3 were augmented by hypertrophic stimuli both in vitro and in vivo. Infection of PARP1 adenovirus induced cardiomyocyte hypertrophy, which could be prevented by STAT3 knockdown or inhibition. Additionally, PARP1 enhanced STAT3 phosphorylation level, nuclear accumulation and transcriptional activity. Mechanistically, PARP1 interacts with STAT3 and retains active phosphorylated-STAT3 in nucleus. In conclusion, our findings provide the first evidence that PARP1 exacerbates cardiac hypertrophy by stabilizing active phosphorylated-STAT3, which suggests that multi-target therapeutic strategies counteracting PARP1 activity and STAT3 activation would be potential for treating cardiovascular diseases.

Published

2017

38. Dkk1 exacerbates doxorubicin-induced cardiotoxicity by inhibiting the Wnt/β-catenin signaling pathway.

Author

Liying Liang, Yalin Tu, Jing Lu, Panxia Wang, Zhen Guo, Qianqian Wang, Kaiteng Guo, Rui Lan, Hong Li, and Peiqing Liu

Subjects

DOXORUBICIN, CARDIOTOXICITY, CATENINS, THERAPEUTICS, HEART injuries, CANCER treatment, CARDIOMYOPATHIES

Abstract

The cancer clinical therapy of doxorubicin (Dox) treatment is limited by its life-threatening cardiotoxic effects. Dickkopf-1 (Dkk1), the founding and best-studied member of the Dkk family, functions as an antagonist of canonical Wnt/β-catenin. Dkk1 is considered to play a broad role in a variety of biological processes, but its effects on Dox-induced cardiomyopathy are poorly understood. Here, we found that the level of Dkk1was significantly increased in Dox-treated groups, and this increase exacerbated Dox-induced cardiomyocyte apoptosis and mitochondrial dysfunction. Overexpressing Dkk1 aggravated Dox-induced cardiotoxicity in H9C2 cells. Similar results were detected when adding active Dkk1 protein extracellularly. Conversely, adding specific antibody blocking extracellular Dkk1 attenuated the cardiotoxic response to Dox. Adenovirus encoding Dkk1 was transduced through intramyocardial injection and exacerbated Dox-induced cardiomyocyte apoptosis, mitochondrial damage and heart injury in vivo. Furthermore, Wnt/β-catenin signaling was inhibited during Dox-induced cardiotoxicity, and the re-activation of β-catenin prevented the effect of overexpressed Dkk1 and Dox-induced cardiotoxicity. In conclusion, these results reveal the crucial role of the Dkk1-Wnt/β-catenin signaling axis in the process of Dox-induced cardiotoxicity and provide novel insights into the potential mechanism of cardiomyopathy caused by clinical application of Dox. [ABSTRACT FROM AUTHOR]

Published

2019

39. Dkk1 exacerbates doxorubicin-induced cardiotoxicity by inhibiting Wnt/β-catenin signaling pathway.

Author

Liying Liang, Yalin Tu, Jing Lu, Panxia Wang, Zhen Guo, Qianqian Wang, Kaiteng Guo, Rui Lan, Hong Li, and Peiqing Liu

Subjects

DOXORUBICIN, CARDIOTOXICITY, CATENINS, HEART injuries, CANCER treatment, CARDIOMYOPATHIES

Abstract

The cancer clinical therapy of Doxorubicin (Dox) is limited by its life-threatening cardiotoxic effects. Dickkopf-1 (Dkk1), the founding member of Dkk family, is best studied and functions as an antagonist of canonical Wnt/ß-catenin. Dkk1 is considered to play a broad role in a variety of biological processes, but its effects on Dox-induced cardiomyopathy is poorly understood. Here, we found that Dkk1 was significantly increased in Dox-treated groups, and this increase exacerbated Dox-induced cardiomyocyte apoptosis and mitochondrial dysfunction. Overexpressing Dkk1 aggravated Dox-induced cardiotoxicity in H9C2 cells. Similar results were detected when adding the Dkk1 active protein extracellularly. Conversely, specific antibody blocking extracellular Dkk1 attenuated Dox-cardiotoxic response. Adenovirus encoding Dkk1 was transduced through intramyocardial injection and exacerbated Dox-induced cardiomyocyte apoptosis, mitochondrial damage and heart injury in vivo. Furthermore, Wnt/ß-catenin signaling was inhibited in Dox-induced cardiotoxicity, the re-activation of ß-catenin relieved overexpressed Dkk1 or Dox-induced cardiotoxicity. In conclusion, these results uncovered that the crucial role of Dkk1-Wnt/ß-catenin signaling axis in the process of Dox-induced cardiotoxicity and provided novel insights into the potential mechanism on cardiomyopathy caused by clinical application of Dox. [ABSTRACT FROM AUTHOR]

Published

2019