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1. Non-contact assessment of cardiac physiology using FO-MVSS-based ballistocardiography: a promising approach for heart failure evaluation

Author

Jing Zhan, Xiaoyan Wu, Xuelei Fu, Chenze Li, Ke-Qiong Deng, Qin Wei, Chao Zhang, Tao Zhao, Congcong Li, Longting Huang, Kewei Chen, Qiongxin Wang, Zhengying Li, and Zhibing Lu

Subjects
Medicine, Science
Abstract

Abstract Continuous monitoring of cardiac motions has been expected to provide essential cardiac physiology information on cardiovascular functioning. A fiber-optic micro-vibration sensing system (FO-MVSS) makes it promising. This study aimed to explore the correlation between Ballistocardiography (BCG) waveforms, measured using an FO-MVSS, and myocardial valve activity during the systolic and diastolic phases of the cardiac cycle in participants with normal cardiac function and patients with congestive heart failure (CHF). A high-sensitivity FO-MVSS acquired continuous BCG recordings. The simultaneous recordings of BCG and electrocardiogram (ECG) signals were obtained from 101 participants to examine their correlation. BCG, ECG, and intracavitary pressure signals were collected from 6 patients undergoing cardiac catheter intervention to investigate BCG waveforms and cardiac cycle phases. Tissue Doppler imaging (TDI) measured cardiac time intervals in 51 participants correlated with BCG intervals. The BCG recordings were further validated in 61 CHF patients to assess cardiac parameters by BCG. For heart failure evaluation machine learning was used to analyze BCG-derived cardiac parameters. Significant correlations were observed between cardiac physiology parameters and BCG's parameters. Furthermore, a linear relationship was found betwen IJ amplitude and cardiac output (r = 0.923, R2 = 0.926, p

Published
2024
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2. TRAF Family Member 4 Promotes Cardiac Hypertrophy Through the Activation of the AKT Pathway

Author

Jian Li, Chang‐Quan Wang, Wen‐Chang Xiao, Yun Chen, Jun Tu, Feng Wan, Ke‐Qiong Deng, and Huo‐Ping Li

Subjects
AKT pathway, cardiac hypertrophy, heart failure, phenylephrine, primary neonatal rat cardiomyocytes, TRAF4, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background Pathological cardiac hypertrophy is a major cause of heart failure morbidity. The complex mechanism of intermolecular interactions underlying the pathogenesis of cardiac hypertrophy has led to a lack of development and application of therapeutic methods. Methods and Results Our study provides the first evidence that TRAF4, a member of the tumor necrosis factor receptor–associated factor (TRAF) family, acts as a promoter of cardiac hypertrophy. Here, Western blotting assays demonstrated that TRAF4 is upregulated in cardiac hypertrophy. Additionally, TRAF4 deletion inhibits the development of cardiac hypertrophy in a mouse model after transverse aortic constriction surgery, whereas its overexpression promotes phenylephrine stimulation‐induced cardiomyocyte hypertrophy in primary neonatal rat cardiomyocytes. Mechanistically, RNA‐seq analysis revealed that TRAF4 promoted the activation of the protein kinase B pathway during cardiac hypertrophy. Moreover, we found that inhibition of protein kinase B phosphorylation rescued the aggravated cardiomyocyte hypertrophic phenotypes caused by TRAF4 overexpression in phenylephrine‐treated neonatal rat cardiomyocytes, suggesting that TRAF4 may regulate cardiac hypertrophy in a protein kinase B–dependent manner. Conclusions Our results revealed the regulatory function of TRAF4 in cardiac hypertrophy, which may provide new insights into developing therapeutic and preventive targets for this disease.

Published
2023
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4. The prevalence of MAFLD and its association with atrial fibrillation in a nationwide health check-up population in China

Author

Fang Lei, Juan-Juan Qin, Xiaohui Song, Ye-Mao Liu, Ming-Ming Chen, Tao Sun, Xuewei Huang, Ke-Qiong Deng, Xiuran Zuo, Dongai Yao, Li-Juan Xu, Huiming Lu, Gang Wang, Feng Liu, Lidong Chen, Jie Luo, Jiahong Xia, Lin Wang, QiongYu Yang, Peng Zhang, Yan-Xiao Ji, Xiao-Jing Zhang, Zhi-Gang She, Qiang Zeng, Hongliang Li, and Jingjing Cai

Subjects
mafld, insulin resistance, prevalence, atrial fibrillation, association, Diseases of the endocrine glands. Clinical endocrinology, RC648-665
Abstract

Background and aimsThe epidemiological characteristics of MAFLD and its relationship with atrial fibrillation (AF) are limited in China. Therefore, we explored the epidemiological characteristics of MAFLD from adults along with the association of MAFLD and 12-ECG diagnosed AF in a nationwide population from health check-up centers.MethodsThis observational study used cross-sectional and longitudinal studies with 2,083,984 subjects from 2009 to 2017. Age-, sex-, and regional-standardized prevalence of MAFLD was estimated. Latent class analysis (LCA) was used to identify subclusters of MAFLD. Multivariable logistic regression and mixed-effects Cox regression models were used to analyze the relationship between MAFLD and AF.ResultsThe prevalence of MAFLD increased from 22.75% to 35.58% during the study period, with higher rates in males and populations with high BMI or resided in northern regions. The MAFLD population was clustered into three classes with different metabolic features by LCA. Notably, a high proportion of MAFLD patients in all clusters had overweight and prediabetes or diabetes. The MAFLD was significantly associated with a higher risk of AF in the cross-sectional study and in the longitudinal study. In addition, the coexistence of prediabetes or diabetes had the largest impact on subsequent AF.ConclusionOur findings suggested a high prevalence of MAFLD and a high prevalence of other metabolic diseases in the MAFLD population, particularly overweight and glucose dysregulation. Moreover, MAFLD was associated with a significantly higher risk for existing and subsequent subclinical AF in the Chinese population.

Published
2022
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5. Cardiac Involvement in Recovered Patients From COVID-19: A Preliminary 6-Month Follow-Up Study

Author

Xiaoyan Wu, Ke-Qiong Deng, Chenze Li, Zhaoxia Yang, Huijuan Hu, Huanhuan Cai, Chao Zhang, Tao He, Fang Zheng, Hairong Wang, Xin A. Zhang, Antoine Caillon, Yufeng Yuan, Xinghuan Wang, Haibo Xu, and Zhibing Lu

Subjects
cardiac magnetic resonance imaging, fibrosis, follow-up, cardiac injury, COVID-19, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background: Accumulating evidence has revealed that coronavirus disease 2019 (COVID-19) patients may be complicated with myocardial injury during hospitalization. However, data regarding persistent cardiac involvement in patients who recovered from COVID-19 are limited. Our goal is to further explore the sustained impact of COVID-19 during follow-up, focusing on the cardiac involvement in the recovered patients.Methods: In this prospective observational follow-up study, we enrolled a total of 40 COVID-19 patients (20 with and 20 without cardiac injury during hospitalization) who were discharged from Zhongnan Hospital of Wuhan University for more than 6 months, and 27 patients (13 with and 14 without cardiac injury during hospitalization) were finally included in the analysis. Clinical information including self-reported symptoms, medications, laboratory findings, Short Form 36-item scores, 6-min walk test, clinical events, electrocardiogram assessment, echocardiography measurement, and cardiac magnetic resonance imaging was collected and analyzed.Results: Among 27 patients finally included, none of patients reported any obvious cardiopulmonary symptoms at the 6-month follow-up. There were no statistically significant differences in terms of the quality of life and exercise capacity between the patients with and without cardiac injury. No significant abnormalities were detected in electrocardiogram manifestations in both groups, except for nonspecific ST-T changes, premature beats, sinus tachycardia/bradycardia, PR interval prolongation, and bundle-branch block. All patients showed normal cardiac structure and function, without any statistical differences between patients with and without cardiac injury by echocardiography. Compared with patients without cardiac injury, patients with cardiac injury exhibited a significantly higher positive proportion in late gadolinium enhancement sequences [7/13 (53.8%) vs. 1/14 (7.1%), p = 0.013], accompanied by the elevation of circulating ST2 level [median (interquartile range) = 16.6 (12.1, 22.5) vs. 12.5 (9.5, 16.7); p = 0.044]. Patients with cardiac injury presented higher levels of aspartate aminotransferase, creatinine, high-sensitivity troponin I, lactate dehydrogenase, and N-terminal pro–B-type natriuretic peptide than those without cardiac injury, although these indexes were within the normal range for all recovered patients at the 6-month follow-up. Among patients with cardiac injury, patients with positive late gadolinium enhancement presented higher cardiac biomarker (high-sensitivity troponin I) and inflammatory factor (high-sensitivity C-reactive protein) on admission than the late gadolinium enhancement–negative subgroup.Conclusions: Our preliminary 6-month follow-up study with a limited number of patients revealed persistent cardiac involvement in 29.6% (8/27) of recovered patients from COVID-19 after discharge. Patients with cardiac injury during hospitalization were more prone to develop cardiac fibrosis during their recovery. Among patients with cardiac injury, those with relatively higher cardiac biomarkers and inflammatory factors on admission appeared more likely to have cardiac involvement in the convalescence phase.

Published
2021
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6. Association of Statin Use With the In-Hospital Outcomes of 2019-Coronavirus Disease Patients: A Retrospective Study

Author

Yongzhen Fan, Tao Guo, Feifei Yan, Ming Gong, Xin A. Zhang, Chenze Li, Tao He, Huimin Luo, Lin Zhang, Ming Chen, Xiaoyan Wu, Hairong Wang, Ke-Qiong Deng, Jiao Bai, Lin Cai, and Zhibing Lu

Subjects
COVID-19, statin, outcome, mortality, ARDS, Medicine (General), R5-920
Abstract

Background: Statins have multiple protective effects on inflammation, immunity and coagulation, and may help alleviate pneumonia. However, there was no report focusing on the association of statin use with in-hospital outcomes of patients with coronavirus disease 2019 (COVID-19). We investigated the association between the use of statins and in-hospital outcomes of patients with COVID-19.Methods: In this retrospective case series, consecutive COVID-19 patients admitted at 2 hospitals in Wuhan, China, from March 12, 2020 to April 14, 2020 were analyzed. A 1:1 matched cohort was created by propensity score-matched analysis. Demographic data, laboratory findings, comorbidities, treatments and in-hospital outcomes were collected and compared between COVID-19 patients taking and not taking statins.Result: A total of 2,147 patients with COVID-19 were enrolled in this study. Of which, 250 patients were on statin therapy. The mortality was 2.4% (6/250) for patients taking statins while 3.7% (70/1,897) for those not taking statins. In the multivariate Cox model, after adjusting for age, gender, admitted hospital, comorbidities, in-hospital medications and blood lipids, the risk was lower for mortality (adjusted HR, 0.428; 95% CI, 0.169–0.907; P = 0.029), acute respiratory distress syndrome (ARDS) (adjusted HR, 0.371; 95% CI, 0.180–0.772; P = 0.008) or intensive care unit (ICU) care (adjusted HR, 0.319; 95% CI, 0.270–0.945; P = 0.032) in the statin group vs. the non-statin group. After propensity score-matched analysis based on 18 potential confounders, a 1:1 matched cohort (206:206) was created. In the matched cohort, the Kaplan-Meier survival curves showed that the use of statins was associated with better survival (P = 0.025). In a Cox regression model, the use of statins was associated with lower risk of mortality (unadjusted HR, 0.254; 95% CI, 0.070–0.926; P = 0.038), development of ARDS (unadjusted HR, 0.240; 95% CI, 0.087–0.657; P = 0.006), and admission of ICU (unadjusted HR, 0.349; 95% CI, 0.150–0.813; P = 0.015). The results remained consistent when being adjusted for age, gender, total cholesterol, triglyceride, low density lipoprotein cholesterol, procalcitonin, and brain natriuretic peptide. The favorable outcomes in statin users remained statistically significant in the first sensitivity analysis with comorbid diabetes being excluded in matching and in the second sensitivity analysis with chronic obstructive pulmonary disease being added in matching.Conclusion: In this retrospective analysis, the use of statins in COVID-19 patients was associated with better clinical outcomes and is recommended to be continued in patients with COVID-19.

Published
2020
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7. NULP1 Alleviates Cardiac Hypertrophy by Suppressing NFAT3 Transcriptional Activity

Author

Xin Zhang, Fang Lei, Xiao‐Ming Wang, Ke‐Qiong Deng, Yan‐Xiao Ji, Yan Zhang, Hongliang Li, Xiao‐Dong Zhang, Zhibing Lu, and Peng Zhang

Subjects
aortic banding, heart failure, NFAT3 signaling, nuclear localized protein 1, pathological cardiac hypertrophy, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background The development of pathological cardiac hypertrophy involves the coordination of a series of transcription activators and repressors, while their interplay to trigger pathological gene reprogramming remains unclear. NULP1 (nuclear localized protein 1) is a member of the basic helix‐loop‐helix family of transcription factors and its biological functions in pathological cardiac hypertrophy are barely understood. Methods and Results Immunoblot and immunostaining analyses showed that NULP1 expression was consistently reduced in the failing hearts of patients and hypertrophic mouse hearts and rat cardiomyocytes. Nulp1 knockout exacerbates aortic banding‐induced cardiac hypertrophy pathology, which was significantly blunted by transgenic overexpression of Nulp1. Signal pathway screening revealed the nuclear factor of activated T cells (NFAT) pathway to be dramatically suppressed by NULP1. Coimmunoprecipitation showed that NULP1 directly interacted with the topologically associating domain of NFAT3 via its C‐terminal region, which was sufficient to suppress NFAT3 transcriptional activity. Inactivation of the NFAT pathway by VIVIT peptides in vivo rescued the aggravated pathogenesis of cardiac hypertrophy resulting from Nulp1 deficiency. Conclusions NULP1 is an endogenous suppressor of NFAT3 signaling under hypertrophic stress and thus negatively regulates the pathogenesis of cardiac hypertrophy. Targeting overactivated NFAT by NULP1 may be a novel therapeutic strategy for the treatment of pathological cardiac hypertrophy and heart failure.

Published
2020
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8. The ubiquitin E3 ligase TRAF6 exacerbates pathological cardiac hypertrophy via TAK1-dependent signalling

Author

Yan-Xiao Ji, Peng Zhang, Xiao-Jing Zhang, Yi-Chao Zhao, Ke-Qiong Deng, Xi Jiang, Pi-Xiao Wang, Zan Huang, and Hongliang Li

Subjects
Science
Abstract

TRAF6 is a ubiquitin E3 ligase regulating a number of biological processes. Here the authors show that ROS, generated during pathological cardiac stress, induces TRAF6 auto-ubiquitination and activation, promoting its interaction with and ubiquitination of TAK1 that contributes to development of cardiac hypertrophy.

Published
2016
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9. Suppressor of IKKɛ is an essential negative regulator of pathological cardiac hypertrophy

Author

Ke-Qiong Deng, Aibing Wang, Yan-Xiao Ji, Xiao-Jing Zhang, Jing Fang, Yan Zhang, Peng Zhang, Xi Jiang, Lu Gao, Xue-Yong Zhu, Yichao Zhao, Lingchen Gao, Qinglin Yang, Xue-Hai Zhu, Xiang Wei, Jun Pu, and Hongliang Li

Subjects
Science
Abstract

Abstract Although pathological cardiac hypertrophy represents a leading cause of morbidity and mortality worldwide, our understanding of the molecular mechanisms underlying this disease is still poor. Here, we demonstrate that suppressor of IKKɛ (SIKE), a negative regulator of the interferon pathway, attenuates pathological cardiac hypertrophy in rodents and non-human primates in a TANK-binding kinase 1 (TBK1)/AKT-dependent manner. Sike-deficient mice develop cardiac hypertrophy and heart failure, whereas Sike-overexpressing transgenic (Sike-TG) mice are protected from hypertrophic stimuli. Mechanistically, SIKE directly interacts with TBK1 to inhibit the TBK1-AKT signalling pathway, thereby achieving its anti-hypertrophic action. The suppression of cardiac remodelling by SIKE is further validated in rats and monkeys. Collectively, these findings identify SIKE as a negative regulator of cardiac remodelling in multiple animal species due to its inhibitory regulation of the TBK1/AKT axis, suggesting that SIKE may represent a therapeutic target for the treatment of cardiac hypertrophy and heart failure.

Published
2016
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10. Carboxyl‐Terminal Modulator Protein Ameliorates Pathological Cardiac Hypertrophy by Suppressing the Protein Kinase B Signaling Pathway

Author

Xiaoxiong Liu, Qin Yang, Li‐Hua Zhu, Jia Liu, Ke‐Qiong Deng, Xue‐Yong Zhu, Ye Liu, Jun Gong, Peng Zhang, Shuyan Li, Hao Xia, and Zhi‐Gang She

Subjects
angiotensin II, aortic banding, carboxyl‐terminal modulator protein, pathological cardiac hypertrophy, signal transduction, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background Carboxyl‐terminal modulator protein (CTMP) has been implicated in cancer, brain injury, and obesity. However, the role of CTMP in pathological cardiac hypertrophy has not been identified. Methods and Results In this study, decreased expression of CTMP was observed in both human failing hearts and murine hypertrophied hearts. To further explore the potential involvement of CTMP in pathological cardiac hypertrophy, cardiac‐specific CTMP knockout and overexpression mice were generated. In vivo experiments revealed that CTMP deficiency exacerbated the cardiac hypertrophy, fibrosis, and function induced by pressure overload, whereas CTMP overexpression alleviated the response to hypertrophic stimuli. Consistent with the in vivo results, adenovirus‐mediated gain‐of‐function or loss‐of‐function experiments showed that CTMP also exerted a protective effect against hypertrophic responses to angiotensin II in vitro. Mechanistically, CTMP ameliorated pathological cardiac hypertrophy through the blockade of the protein kinase B signaling pathway. Moreover, inhibition of protein kinase B activation with LY294002 rescued the deteriorated effect in aortic banding–treated cardiac‐specific CTMP knockout mice. Conclusions Taken together, these findings imply, for the first time, that increasing the cardiac expression of CTMP may be a novel therapeutic strategy for pathological cardiac hypertrophy.

Published
2018
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13. The E3 Ligase TRIM16 Is a Key Suppressor of Pathological Cardiac Hypertrophy

Author

Jiayi Liu, Wei Li, Ke-Qiong Deng, Song Tian, Hui Liu, Hongjie Shi, Qian Fang, Zhen Liu, Ze Chen, Tian Tian, Shanyu Gan, Fengjiao Hu, Manli Hu, Xu Cheng, Yan-Xiao Ji, Peng Zhang, Zhi-Gang She, Xiao-Jing Zhang, Shaoze Chen, Jingjing Cai, and Hongliang Li

Subjects
Heart Failure, Mice, Knockout, Tripartite Motif Proteins, Disease Models, Animal, Mice, Physiology, Ubiquitin-Protein Ligases, Animals, Cardiomegaly, Myocytes, Cardiac, Cardiology and Cardiovascular Medicine
Abstract

Background: Pathological cardiac hypertrophy is one of the leading causes of heart failure with highly complicated pathogeneses. The E3 ligase TRIM16 (tripartite motif–containing protein 16) has been recognized as a pivotal regulator to control cell survival, immune response, and oxidativestress. However, the role of Trim16 in cardiac hypertrophy is unknown. Methods: We generated cardiac-specific knockout mice and adeno-associated virus serotype 9–Trim16 mice to evaluate the function of Trim16 in pathological myocardial hypertrophy. The direct effect of TRIM16 on cardiomyocyte enlargement was examined using an adenovirus system. Furthermore, we combined RNA-sequencing and interactome analysis that was followed by multiple molecular biological methodologies to identify the direct target and corresponding molecular events contributing to TRIM16 function. Results: We found an intimate correlation of Trim16 expression with hypertrophy-related heart failure in both human and mouse. Our functional investigations and unbiased transcriptomic analyses clearly demonstrated that Trim16 deficiency markedly exacerbated cardiomyocyte enlargement in vitro and in transverse aortic constriction–induced cardiac hypertrophy mouse model, whereas Trim16 overexpression attenuated cardiac hypertrophy and remodeling. Mechanistically, Prdx1 (peroxiredoxin 1) is an essential target of Trim16 in cardiac hypertrophy. We found that Trim16 interacts with Prdx1 and inhibits its phosphorylation, leading to a robust enhancement of its downstream Nrf2 (nuclear factor–erythroid 2–related factor 2) pathway to block cardiac hypertrophy. Trim16-blocked Prdx1 phosphorylation was largely dependent on a direct interaction between Trim16 and Src and the resultant Src ubiquitinational degradation. Notably, Prdx1 knockdown largely abolished the anti-hypertrophic effects of Trim16 overexpression. Conclusions: Our findings provide the first evidence supporting Trim16 as a novel suppressor of pathological cardiac hypertrophy and indicate that targeting the Trim16-Prdx1 axis represents a promising therapeutic strategy for hypertrophy-related heart failure.

Published
2022

14. Role of hepatic lipid species in the progression of nonalcoholic fatty liver disease

Author

Ke-Qiong Deng, Xuewei Huang, Fang Lei, Xiao-Jing Zhang, Peng Zhang, Zhi-Gang She, Jingjing Cai, Yan-Xiao Ji, and Hongliang Li

Subjects
Liver, Physiology, Non-alcoholic Fatty Liver Disease, Fatty Acids, Lipidomics, Humans, Cell Biology, Lipid Metabolism
Abstract

Nonalcoholic fatty liver disease (NAFLD) has become the most common liver disease due to the global pandemic of metabolic diseases. Dysregulation of hepatic lipid metabolism plays a central role in the initiation and progression of NAFLD. With the advancement of lipidomics, an increasing number of lipid species and underlying mechanisms associating hepatic lipid components have been revealed. Therefore, the focus of this review is to highlight the links between hepatic lipid species and their mechanisms mediating the pathogenesis of NAFLD. We first summarized the interplay between NAFLD and hepatic lipid disturbances. Next, we focused on reviewing the role of saturated fatty acids, cholesterol, oxidized phospholipids, and their respective intermediates in the pathogenesis of NAFLD. The mechanisms by which monounsaturated fatty acids and other pro-resolving mediators exert protective effects are also addressed. Finally, we further discussed the implication of different analysis approaches in lipidomics. Evolving insights into the pathophysiology of NAFLD will provide the opportunity for drug development.

Published
2022

15. Energy substrate metabolism and oxidative stress in metabolic cardiomyopathy

Author

Ze Chen, Zhao-Xia Jin, Jingjing Cai, Ruyan Li, Ke-Qiong Deng, Yan-Xiao Ji, Fang Lei, Huo-Ping Li, Zhibing Lu, and Hongliang Li

Subjects
Oxidative Stress, Myocardium, Drug Discovery, Molecular Medicine, Humans, Reactive Oxygen Species, Cardiomyopathies, Energy Metabolism, Genetics (clinical)
Abstract

Metabolic cardiomyopathy is an emerging cause of heart failure in patients with obesity, insulin resistance, and diabetes. It is characterized by impaired myocardial metabolic flexibility, intramyocardial triglyceride accumulation, and lipotoxic damage in association with structural and functional alterations of the heart, unrelated to hypertension, coronary artery disease, and other cardiovascular diseases. Oxidative stress plays an important role in the development and progression of metabolic cardiomyopathy. Mitochondria are the most significant sources of reactive oxygen species (ROS) in cardiomyocytes. Disturbances in myocardial substrate metabolism induce mitochondrial adaptation and dysfunction, manifested as a mismatch between mitochondrial fatty acid oxidation and the electron transport chain (ETC) activity, which facilitates ROS production within the ETC components. In addition, non-ETC sources of mitochondrial ROS, such as β-oxidation of fatty acids, may also produce a considerable quantity of ROS in metabolic cardiomyopathy. Augmented ROS production in cardiomyocytes can induce a variety of effects, including the programming of myocardial energy substrate metabolism, modulation of metabolic inflammation, redox modification of ion channels and transporters, and cardiomyocyte apoptosis, ultimately leading to the structural and functional alterations of the heart. Based on the above mechanistic views, the present review summarizes the current understanding of the mechanisms underlying metabolic cardiomyopathy, focusing on the role of oxidative stress.

Published
2022

16. Ca 2+ -Dependent NOX5 (NADPH Oxidase 5) Exaggerates Cardiac Hypertrophy Through Reactive Oxygen Species Production

Author

Shan Ouyang, Guo-Jun Zhao, Changjiang Zhang, Zhi-Gang She, Xueyong Zhu, Augusto C. Montezano, Rhian M. Touyz, Fengjiao Hu, Lihua Zhu, Xiao-Jing Zhang, Song Tian, Xiaolan Liu, Chang-Ling Zhao, Ke-Qiong Deng, Yan-Xiao Ji, Peng Zhang, and Hongliang Li

Subjects
0301 basic medicine, Pressure overload, medicine.medical_specialty, NADPH oxidase, biology, Chemistry, 030204 cardiovascular system & hematology, medicine.disease, Left ventricular hypertrophy, medicine.disease_cause, Angiotensin II, Muscle hypertrophy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, Internal medicine, Heart failure, cardiovascular system, Internal Medicine, biology.protein, medicine, MYH7, Oxidative stress
Abstract

NOX5 (NADPH oxidase 5) is a homolog of the gp91 phox subunit of the phagocyte NOX, which generates reactive oxygen species. NOX5 is involved in sperm motility and vascular contraction and has been implicated in diabetic nephropathy, atherosclerosis, and stroke. The function of NOX5 in the cardiac hypertrophy is unknown. Because NOX5 is a Ca 2+ -sensitive, procontractile NOX isoform, we questioned whether it plays a role in cardiac hypertrophy. Studies were performed in (1) cardiac tissue from patients undergoing heart transplant for cardiomyopathy and heart failure, (2) NOX5-expressing rat cardiomyocytes, and (3) mice expressing human NOX5 in a cardiomyocyte-specific manner. Cardiac hypertrophy was induced in mice by transverse aorta coarctation and Ang II (angiotensin II) infusion. NOX5 expression was increased in human failing hearts. Rat cardiomyocytes infected with adenoviral vector encoding human NOX5 cDNA exhibited elevated reactive oxygen species levels with significant enlargement and associated increased expression of ANP (atrial natriuretic peptides) and β-MHC (β-myosin heavy chain) and prohypertrophic genes ( Nppa , Nppb , and Myh7 ) under Ang II stimulation. These effects were reduced by N-acetylcysteine and diltiazem. Pressure overload and Ang II infusion induced left ventricular hypertrophy, interstitial fibrosis, and contractile dysfunction, responses that were exaggerated in cardiac-specific NOX5 trangenic mice. These phenomena were associated with increased reactive oxygen species levels and activation of redox-sensitive MAPK (mitogen-activated protein kinase). N-acetylcysteine treatment reduced cardiac oxidative stress and attenuated cardiac hypertrophy in NOX5 trangenic. Our study defines Ca 2+ -regulated NOX5 as an important NOX isoform involved in oxidative stress- and MAPK-mediated cardiac hypertrophy and contractile dysfunction.

Published
2020

18. Hepatic Interferon Regulatory Factor 6 Alleviates Liver Steatosis and Metabolic Disorder by Transcriptionally Suppressing Peroxisome Proliferator‐Activated Receptor γ in Mice

Author

Xu Cheng, Ke-Qiong Deng, Jingjing Cai, Zhi-Gang She, Zan Huang, Hongliang Li, Wen-Zhi He, Lei Zhang, Cuijuan Han, Song Tian, Hui-Fen Fan, Peng Zhang, Jingjing Tong, Ye Liu, Jia-Zhen Zhang, and Guo-Jun Zhao

Subjects
Male, 0301 basic medicine, Down-Regulation, Peroxisome proliferator-activated receptor, Mice, Transgenic, Biology, Diet, High-Fat, Sensitivity and Specificity, Mice, Random Allocation, 03 medical and health sciences, 0302 clinical medicine, Non-alcoholic Fatty Liver Disease, Nonalcoholic fatty liver disease, medicine, Animals, Humans, Mice, Knockout, chemistry.chemical_classification, Hepatology, Fatty liver, Metabolic disorder, Lipid metabolism, DNA Methylation, Lipid Metabolism, medicine.disease, Mice, Inbred C57BL, PPAR gamma, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, chemistry, Interferon Regulatory Factors, Lipogenesis, Hepatocytes, Cancer research, 030211 gastroenterology & hepatology, Steatosis, Interferon regulatory factors
Abstract

Nonalcoholic fatty liver disease (NAFLD) has become a worldwide epidemic. A large and growing unmet therapeutic need has inspired numerous studies in the field. Integrating the published genomic data available in the Gene Expression Omnibus (GEO) with NAFLD samples from rodents, we discovered that interferon regulatory factor 6 (IRF6) is significantly downregulated in high-fat diet (HFD)-induced fatty liver. In the current study, we identified IRF6 in hepatocytes as a protective factor in liver steatosis (LS). During HFD challenge, hepatic Irf6 was suppressed by promoter hypermethylation. Severity of HFD-induced LS was exacerbated in hepatocyte-specific Irf6 knockout mice, whereas hepatocyte-specific transgenic mice overexpressing Irf6 (IRF6-HTG) exhibited alleviated steatosis and metabolic disorder in response to HFD feeding. Mechanistic studies in vitro demonstrated that hepatocyte IRF6 directly binds to the promoter of the peroxisome proliferator-activated receptor γ (PPARγ) gene and subsequently halts the transcription of Pparγ and its target genes (e.g., genes that regulate lipogenesis and lipid acid uptake) under physiological conditions. Conclusion: Irf6 is downregulated by promoter hypermethylation upon metabolic stimulus exposure, which fail to inhibit Pparγ and its targets, driving abnormalities of lipid metabolism.

Published
2019

19. Cardiac Involvement in Recovered Patients From COVID-19: A Preliminary 6-Month Follow-Up Study

Author

Haibo Xu, Huijuan Hu, Tao He, Xiaoyan Wu, Chao Zhang, Hairong Wang, Yufeng Yuan, Zhaoxia Yang, Ke-Qiong Deng, Huanhuan Cai, Antoine Caillon, Zhibing Lu, Chenze Li, Fang Zheng, Xin A Zhang, and Xinghuan Wang

Subjects
Bradycardia, medicine.medical_specialty, cardiac injury, Cardiac fibrosis, Sinus tachycardia, media_common.quotation_subject, cardiac magnetic resonance imaging, 030204 cardiovascular system & hematology, Cardiovascular Medicine, 03 medical and health sciences, 0302 clinical medicine, Interquartile range, Cardiac magnetic resonance imaging, Internal medicine, Troponin I, medicine, follow-up, Diseases of the circulatory (Cardiovascular) system, 030212 general & internal medicine, PR interval, media_common, Original Research, medicine.diagnostic_test, business.industry, Convalescence, fibrosis, COVID-19, medicine.disease, RC666-701, Cardiology, cardiovascular system, medicine.symptom, Cardiology and Cardiovascular Medicine, business
Abstract

Background: Accumulating evidence has revealed that coronavirus disease 2019 (COVID-19) patients may be complicated with myocardial injury during hospitalization. However, data regarding persistent cardiac involvement in patients who recovered from COVID-19 are limited. Our goal is to further explore the sustained impact of COVID-19 during follow-up, focusing on the cardiac involvement in the recovered patients.Methods: In this prospective observational follow-up study, we enrolled a total of 40 COVID-19 patients (20 with and 20 without cardiac injury during hospitalization) who were discharged from Zhongnan Hospital of Wuhan University for more than 6 months, and 27 patients (13 with and 14 without cardiac injury during hospitalization) were finally included in the analysis. Clinical information including self-reported symptoms, medications, laboratory findings, Short Form 36-item scores, 6-min walk test, clinical events, electrocardiogram assessment, echocardiography measurement, and cardiac magnetic resonance imaging was collected and analyzed.Results: Among 27 patients finally included, none of patients reported any obvious cardiopulmonary symptoms at the 6-month follow-up. There were no statistically significant differences in terms of the quality of life and exercise capacity between the patients with and without cardiac injury. No significant abnormalities were detected in electrocardiogram manifestations in both groups, except for nonspecific ST-T changes, premature beats, sinus tachycardia/bradycardia, PR interval prolongation, and bundle-branch block. All patients showed normal cardiac structure and function, without any statistical differences between patients with and without cardiac injury by echocardiography. Compared with patients without cardiac injury, patients with cardiac injury exhibited a significantly higher positive proportion in late gadolinium enhancement sequences [7/13 (53.8%) vs. 1/14 (7.1%), p = 0.013], accompanied by the elevation of circulating ST2 level [median (interquartile range) = 16.6 (12.1, 22.5) vs. 12.5 (9.5, 16.7); p = 0.044]. Patients with cardiac injury presented higher levels of aspartate aminotransferase, creatinine, high-sensitivity troponin I, lactate dehydrogenase, and N-terminal pro–B-type natriuretic peptide than those without cardiac injury, although these indexes were within the normal range for all recovered patients at the 6-month follow-up. Among patients with cardiac injury, patients with positive late gadolinium enhancement presented higher cardiac biomarker (high-sensitivity troponin I) and inflammatory factor (high-sensitivity C-reactive protein) on admission than the late gadolinium enhancement–negative subgroup.Conclusions: Our preliminary 6-month follow-up study with a limited number of patients revealed persistent cardiac involvement in 29.6% (8/27) of recovered patients from COVID-19 after discharge. Patients with cardiac injury during hospitalization were more prone to develop cardiac fibrosis during their recovery. Among patients with cardiac injury, those with relatively higher cardiac biomarkers and inflammatory factors on admission appeared more likely to have cardiac involvement in the convalescence phase.

Published
2021

20. NULP1 Alleviates Cardiac Hypertrophy by Suppressing NFAT3 Transcriptional Activity

Author

Yan-Xiao Ji, Peng Zhang, Xiaoming Wang, Yan Zhang, Xiao-Dong Zhang, Hongliang Li, Zhibing Lu, Fang Lei, Ke-Qiong Deng, and Xin Zhang

Subjects
Transcription, Genetic, Transgene, Endogeny, Cardiomegaly, Mice, Transgenic, aortic banding, 030204 cardiovascular system & hematology, Pathogenesis, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, nuclear localized protein 1, 0302 clinical medicine, NFAT Pathway, medicine, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, Immunoprecipitation, Myocytes, Cardiac, Transcription factor, 030304 developmental biology, Original Research, Mice, Knockout, Heart Failure, 0303 health sciences, NFATC Transcription Factors, business.industry, NFAT, Hypertrophy, medicine.disease, Phosphoric Monoester Hydrolases, Remodeling, Cell biology, Rats, NFAT3 signaling, Repressor Proteins, Echocardiography, Heart failure, cardiovascular system, pathological cardiac hypertrophy, Cardiology and Cardiovascular Medicine, business, Oligopeptides, Immunostaining, Gene Deletion
Abstract

Background The development of pathological cardiac hypertrophy involves the coordination of a series of transcription activators and repressors, while their interplay to trigger pathological gene reprogramming remains unclear. NULP1 (nuclear localized protein 1) is a member of the basic helix‐loop‐helix family of transcription factors and its biological functions in pathological cardiac hypertrophy are barely understood. Methods and Results Immunoblot and immunostaining analyses showed that NULP1 expression was consistently reduced in the failing hearts of patients and hypertrophic mouse hearts and rat cardiomyocytes. Nulp1 knockout exacerbates aortic banding‐induced cardiac hypertrophy pathology, which was significantly blunted by transgenic overexpression of Nulp1 . Signal pathway screening revealed the nuclear factor of activated T cells (NFAT) pathway to be dramatically suppressed by NULP1. Coimmunoprecipitation showed that NULP1 directly interacted with the topologically associating domain of NFAT3 via its C‐terminal region, which was sufficient to suppress NFAT3 transcriptional activity. Inactivation of the NFAT pathway by VIVIT peptides in vivo rescued the aggravated pathogenesis of cardiac hypertrophy resulting from Nulp1 deficiency. Conclusions NULP1 is an endogenous suppressor of NFAT3 signaling under hypertrophic stress and thus negatively regulates the pathogenesis of cardiac hypertrophy. Targeting overactivated NFAT by NULP1 may be a novel therapeutic strategy for the treatment of pathological cardiac hypertrophy and heart failure.

Published
2020

21. Ca

Author

Guo-Jun, Zhao, Chang-Ling, Zhao, Shan, Ouyang, Ke-Qiong, Deng, Lihua, Zhu, Augusto C, Montezano, Changjiang, Zhang, Fengjiao, Hu, Xue-Yong, Zhu, Song, Tian, Xiaolan, Liu, Yan-Xiao, Ji, Peng, Zhang, Xiao-Jing, Zhang, Zhi-Gang, She, Rhian M, Touyz, and Hongliang, Li

Subjects
Mitogen-Activated Protein Kinase Kinases, Phagocytes, Angiotensin II, Cardiomegaly, Mice, Transgenic, Free Radical Scavengers, Acetylcysteine, Rats, Isoenzymes, Ventricular Myosins, Mice, Oxidative Stress, Gene Expression Regulation, NADPH Oxidase 5, Animals, Humans, Vasoconstrictor Agents, Myocytes, Cardiac, Reactive Oxygen Species, Signal Transduction
Abstract

NOX5 (NADPH oxidase 5) is a homolog of the gp91

Published
2020

22. Clinical Characteristics And Risk Factors For Fatal Outcome in Patients With 2019-Coronavirus Infected Disease (COVID-19) in Wuhan, China

Author

Zhibing Lu, Ke-Qiong Deng, Xiaoyan Wu, Hairong Wang, Lin Zhang, Huimin Luo, Jing Wan, Ming Chen, Yao Gong, Xinghuan Wang, Jianlei Cao, Yongzhen Fan, Tao He, and Tao Guo

Subjects
2019-20 coronavirus outbreak, Fatal outcome, Coronavirus disease 2019 (COVID-19), business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), medicine, In patient, Disease, medicine.disease_cause, China, business, Virology, Coronavirus
Abstract

Background: Increasing numbers of confirmed cases and deaths due to 2019-coronavirus infected disease (COVID-19) have occurred in Wuhan, China since December 20

Published
2020

23. Control of Pathological Cardiac Hypertrophy by Transcriptional Corepressor IRF2BP2 (Interferon Regulatory Factor-2 Binding Protein 2)

Author

Tianyu Li, Junhong Guo, Hongliang Li, Yan-Xiao Ji, Chun Fang, Xiao-Jing Zhang, Xiang Wei, Xuehai Zhu, Ke-Qiong Deng, Peng Zhang, and Jing Fang

Subjects
0301 basic medicine, medicine.medical_specialty, Transcription, Genetic, Down-Regulation, Cardiomegaly, Mice, Transgenic, Biology, Transcriptome, Mice, 03 medical and health sciences, Transactivation, Downregulation and upregulation, Internal medicine, Internal Medicine, medicine, Animals, Myocyte, Myocytes, Cardiac, Transcription factor, NFATC Transcription Factors, Gene Expression Profiling, Binding protein, Protective Factors, Angiotensin II, Up-Regulation, Cell biology, Disease Models, Animal, 030104 developmental biology, Endocrinology, Interferon Regulatory Factor 2-Binding Protein 2, Transcription Factors
Abstract

The transcription factor NFAT1 (nuclear factor of activated T-cells 1), with the aid of transcriptional coactivators, has been recognized for its necessity and sufficiency to drive pathological cardiac hypertrophy. However, how the transcriptional activity of NFAT1 in terms of cardiac hypertrophy is controlled at the transcriptional level has not been well defined. Herein, we showed that a cardiac-enriched protein IRF2BP2 (interferon regulatory factor-2 binding protein 2) was further upregulated in both human and mouse hypertrophied myocardium and negatively regulated cardiomyocyte hypertrophic response in vitro. By generating cardiomyocyte-specific Irf2bp2 knockout and Irf2bp2 -transgenic mouse strains, our in vivo experiments showed that, whereas IRF2BP2 loss-of-function exacerbated both aortic banding- and angiotensin II infusion-induced cardiac hypertrophic response, IRF2BP2 overexpression exerted a strong protective effect against these maladaptive processes. Particularly, IRF2BP2 directly interacted with the C-terminal transactivation domain of NFAT1 by competing with myocyte enhancer factor-2C and disturbing their transcriptional synergism, thereby impeding NFAT1-transactivated hypertrophic transcriptome. As a result, the devastating effect of Irf2bp2 deficiency on cardiac hypertrophy was largely rescued by NFAT1 blockage. Our study, thus, defined IRF2BP2 as a novel negative regulator in controlling pathological cardiac hypertrophy at the transcriptional level.

Published
2017

24. Tripartite Motif 8 Contributes to Pathological Cardiac Hypertrophy Through Enhancing Transforming Growth Factor β–Activated Kinase 1–Dependent Signaling Pathways

Author

Mei Fanghua, Xi Jiang, Pi-Xiao Wang, Jia Huang, Lijuan Chen, Hongliang Li, Yan-Xiao Ji, Ke-Qiong Deng, and Genshan Ma

Subjects
0301 basic medicine, Ubiquitin-Protein Ligases, Cardiomegaly, Nerve Tissue Proteins, 030204 cardiovascular system & hematology, Mice, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, Internal Medicine, Animals, Humans, Myocytes, Cardiac, Pathological, Cells, Cultured, Adaptor Proteins, Signal Transducing, biology, Kinase, Gene Expression Regulation, Developmental, Angiotensin II, Rats, Cell biology, Ubiquitin ligase, Disease Models, Animal, 030104 developmental biology, Animals, Newborn, biology.protein, RNA, Signal transduction, Carrier Proteins, Function (biology), Signal Transduction, Transforming growth factor
Abstract

Tripartite motif (TRIM) 8 functions as an E3 ubiquitin ligase, interacting with and ubiquitinating diverse substrates, and is implicated in various pathological processes. However, the function of TRIM8 in the heart remains largely uncharacterized. This study aims to explore the role of TRIM8 in the development of pathological cardiac hypertrophy. Mice and isolated neonatal rat cardiomyocytes overexpressing or lacking TRIM8 were examined in several experiments. The effect of aortic banding–induced cardiac hypertrophy was analyzed by echocardiographic, pathological and molecular analyses. Our results indicated that the TRIM8 overexpression in hearts exacerbated the cardiac hypertrophy triggered by aortic banding. In contrast, the development of pathological cardiac hypertrophy was profoundly blocked in TRIM8-deficient hearts. Mechanistically, our study suggests that TRIM8 may elicit cardiodetrimental effects by promoting the activation of transforming growth factor β–activated kinase 1 (TAK1)-p38/JNK signaling pathways. Similar results were observed in cultured neonatal rat cardiomyocytes treated with angiotensin II. The rescue experiments using the TAK1-specific inhibitor 5z-7-ox confirmed the requirement of TAK1 activation in TRIM8-mediated pathological cardiac hypertrophy. Furthermore, TRIM8 contributed to TAK1 activation by binding to and promoting TAK1 ubiquitination. In conclusion, our study demonstrates that TRIM8 plays a deleterious role in pressure overload–induced cardiac hypertrophy by accelerating the activation of TAK1-dependent signaling pathways.

Published
2017

25. The ubiquitin E3 ligase TRAF6 exacerbates pathological cardiac hypertrophy via TAK1-dependent signalling

Author

Ke-Qiong Deng, Yichao Zhao, Xiao-Jing Zhang, Xi Jiang, Zan Huang, Yan-Xiao Ji, Pi-Xiao Wang, Peng Zhang, and Hongliang Li

Subjects
0301 basic medicine, medicine.medical_specialty, Ubiquitin-Protein Ligases, Science, General Physics and Astronomy, Cardiomegaly, Mice, Transgenic, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Rats, Sprague-Dawley, 03 medical and health sciences, Ubiquitin, Internal medicine, medicine, Animals, Humans, Cells, Cultured, Mice, Knockout, TNF Receptor-Associated Factor 6, Pressure overload, Multidisciplinary, MAP kinase kinase kinase, Kinase, Ubiquitination, General Chemistry, MAP Kinase Kinase Kinases, Angiotensin II, Ubiquitin ligase, Cell biology, Mice, Inbred C57BL, HEK293 Cells, 030104 developmental biology, Endocrinology, Animals, Newborn, biology.protein, Signal transduction, Protein Binding, Signal Transduction, Transforming growth factor
Abstract

Tumour necrosis factor receptor-associated factor 6 (TRAF6) is a ubiquitin E3 ligase that regulates important biological processes. However, the role of TRAF6 in cardiac hypertrophy remains unknown. Here, we show that TRAF6 levels are increased in human and murine hypertrophied hearts, which is regulated by reactive oxygen species (ROS) production. Cardiac-specific Traf6 overexpression exacerbates cardiac hypertrophy in response to pressure overload or angiotensin II (Ang II) challenge, whereas Traf6 deficiency causes an alleviated hypertrophic phenotype in mice. Mechanistically, we show that ROS, generated during hypertrophic progression, triggers TRAF6 auto-ubiquitination that facilitates recruitment of TAB2 and its binding to transforming growth factor beta-activated kinase 1 (TAK1), which, in turn, enables the direct TRAF6–TAK1 interaction and promotes TAK1 ubiquitination. The binding of TRAF6 to TAK1 and the induction of TAK1 ubiquitination and activation are indispensable for TRAF6-regulated cardiac remodelling. Taken together, we define TRAF6 as an essential molecular switch leading to cardiac hypertrophy in a TAK1-dependent manner., TRAF6 is a ubiquitin E3 ligase regulating a number of biological processes. Here the authors show that ROS, generated during pathological cardiac stress, induces TRAF6 auto-ubiquitination and activation, promoting its interaction with and ubiquitination of TAK1 that contributes to development of cardiac hypertrophy.

Published
2016

26. Metformin Is Associated with Higher Incidence of Acidosis, but Not Mortality, in Individuals with COVID-19 and Pre-existing Type 2 Diabetes

Author

Yufeng Yuan, Xuewei Huang, Ke-Qiong Deng, Xu Cheng, Ze Chen, Feng Zhou, Lijin Lin, Xiang Wei, Jingjing Cai, Ming-Ming Chen, Xiao-Jing Zhang, Xiaodong Huang, Jiahong Xia, Juan-Juan Qin, Weiming Mao, Xiaohui Song, Weifang Liu, Zhi-Gang She, Ye-Mao Liu, Peng Zhang, Meng Xia, Bing-Hong Zhang, Hongliang Li, Ping Ye, Yibin Wang, Jiao Guo, Juan Yang, Fang Lei, Yan-Xiao Ji, Xin-Liang Ma, Haomiao Li, Zhibing Lu, Xin Zhang, Qingbo Xu, and Lihua Zhu

Subjects
Male, 0301 basic medicine, endocrine system diseases, Physiology, Type 2 diabetes, Medical Biochemistry and Metabolomics, Kidney, 0302 clinical medicine, Viral, Acidosis, Coronavirus disease 2019, treatment, Lactic, Incidence (epidemiology), Diabetes, Middle Aged, Metformin, Hospitalization, 6.1 Pharmaceuticals, Cohort, Acidosis, Lactic, Female, acidosis, medicine.symptom, Coronavirus Infections, Type 2, medicine.drug, China, medicine.medical_specialty, Pneumonia, Viral, Renal function, Article, coronavirus disease 2019, Endocrinology & Metabolism, 03 medical and health sciences, Commentaries, Internal medicine, Diabetes Mellitus, medicine, Humans, Mortality, Pandemics, Molecular Biology, Metabolic and endocrine, Retrospective Studies, Aged, Inflammation, business.industry, Evaluation of treatments and therapeutic interventions, COVID-19, nutritional and metabolic diseases, Retrospective cohort study, Pneumonia, Cell Biology, medicine.disease, mortality, Treatment, Good Health and Well Being, 030104 developmental biology, Diabetes Mellitus, Type 2, inflammation, Heart failure, Commentary, Biochemistry and Cell Biology, business, 030217 neurology & neurosurgery
Abstract

Summary The safety and efficacy of anti-diabetic drugs are critical for maximizing the benefical impacts of well-controlled blood glucose on the prognosis of individuals with COVID-19 and pre-existing type 2 diabetes (T2D). Metformin is the most commonly prescribed first-line medication for T2D, but its impact on the outcomes of individuals with COVID-19 and T2D remains to be clarified. Our current retrospective study in a cohort of 1,213 hospitalized individuals with COVID-19 and pre-existing T2D indicated that metformin use was significantly associated with a higher incidence of acidosis, particularly in cases with severe COVID-19, but not with 28-day COVID-19-related mortality. Furthermore, metformin use was significantly associated with reduced heart failure and inflammation. Our findings provide clinical evidence in support of continuing metformin treatment in individuals with COVID-19 and pre-existing T2D, but acidosis and kidney function should be carefully monitored in individuals with severe COVID-19., Graphical Abstract, Highlight ● A retrospective study of 1,213 patients on metformin with COVID-19 was performed ● Metformin was associated with increased incidence of acidosis in such patients ● Metformin was not associated with increased 28-day all-cause mortality in the patients ● Metformin was significantly associated with reduced heart failure and inflammation, In a cohort of 1,213 hospitalized patients with COVID-19 and pre-existing type 2 diabetes, Cheng et al. show that metformin use is significantly associated with higher incidence of acidosis, particularly in cases with severe COVID-19, but not with 28-day all-cause mortality. They also found that metformin use is significantly associated with reduced heart failure and inflammation.

Published
2020

27. Carboxyl‐Terminal Modulator Protein Ameliorates Pathological Cardiac Hypertrophy by Suppressing the Protein Kinase B Signaling Pathway

Author

Shuyan Li, Jia Liu, Jun Gong, Lihua Zhu, Ke-Qiong Deng, Xueyong Zhu, Qin Yang, Hao Xia, Peng Zhang, Ye Liu, Zhi-Gang She, and Xiaoxiong Liu

Subjects
Male, 0301 basic medicine, aortic banding, angiotensin II, Ventricular Function, Left, Rats, Sprague-Dawley, carboxyl‐terminal modulator protein, 03 medical and health sciences, chemistry.chemical_compound, In vivo, Fibrosis, Animals, Humans, Medicine, Myocytes, Cardiac, LY294002, Cells, Cultured, Adaptor Proteins, Signal Transducing, Original Research, Mice, Knockout, Heart Failure, Pressure overload, Ventricular Remodeling, business.industry, Membrane Proteins, Hypertrophy, medicine.disease, Angiotensin II, Remodeling, Cell biology, Disease Models, Animal, 030104 developmental biology, Palmitoyl-CoA Hydrolase, chemistry, Protein kinase B signaling, Knockout mouse, pathological cardiac hypertrophy, Hypertrophy, Left Ventricular, Thiolester Hydrolases, Signal transduction, Carrier Proteins, Cardiology and Cardiovascular Medicine, business, Proto-Oncogene Proteins c-akt, signal transduction
Abstract

Background Carboxyl‐terminal modulator protein ( CTMP ) has been implicated in cancer, brain injury, and obesity. However, the role of CTMP in pathological cardiac hypertrophy has not been identified. Methods and Results In this study, decreased expression of CTMP was observed in both human failing hearts and murine hypertrophied hearts. To further explore the potential involvement of CTMP in pathological cardiac hypertrophy, cardiac‐specific CTMP knockout and overexpression mice were generated. In vivo experiments revealed that CTMP deficiency exacerbated the cardiac hypertrophy, fibrosis, and function induced by pressure overload, whereas CTMP overexpression alleviated the response to hypertrophic stimuli. Consistent with the in vivo results, adenovirus‐mediated gain‐of‐function or loss‐of‐function experiments showed that CTMP also exerted a protective effect against hypertrophic responses to angiotensin II in vitro. Mechanistically, CTMP ameliorated pathological cardiac hypertrophy through the blockade of the protein kinase B signaling pathway. Moreover, inhibition of protein kinase B activation with LY 294002 rescued the deteriorated effect in aortic banding–treated cardiac‐specific CTMP knockout mice. Conclusions Taken together, these findings imply, for the first time, that increasing the cardiac expression of CTMP may be a novel therapeutic strategy for pathological cardiac hypertrophy.

Published
2018

28. Mindin regulates vascular smooth muscle cell phenotype and prevents neointima formation

Author

Yan Zhang, Xiao-Jing Zhang, Peng Zhang, Hongliang Li, Shu-Min Zhang, Xueyong Zhu, Song Tian, Ling Huang, Lihua Zhu, Hongjing Guan, and Ke-Qiong Deng

Subjects
Male, Neointima, medicine.medical_specialty, Time Factors, Vascular smooth muscle, Intimal hyperplasia, Genotype, Angiogenesis, Myocytes, Smooth Muscle, Biology, Muscle, Smooth, Vascular, Rats, Sprague-Dawley, Glycogen Synthase Kinase 3, Cell Movement, GSK-3, Internal medicine, medicine, Animals, Humans, Protein Kinase Inhibitors, GSK3B, Protein kinase B, Cells, Cultured, PI3K/AKT/mTOR pathway, Cell Proliferation, Mice, Knockout, Extracellular Matrix Proteins, Glycogen Synthase Kinase 3 beta, Cell Differentiation, General Medicine, medicine.disease, Rats, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, Phenotype, Endocrinology, Gene Expression Regulation, Rats, Transgenic, Carotid Artery Injuries, Proto-Oncogene Proteins c-akt, Signal Transduction
Abstract

Mindin/spondin 2, an extracellular matrix (ECM) component that belongs to the thrombospondin type 1 (TSR) class of molecules, plays prominent roles in the regulation of inflammatory responses, angiogenesis and metabolic disorders. Our most recent studies indicated that mindin is largely involved in the initiation and development of cardiac and cerebrovascular diseases [Zhu et al. (2014) J. Hepatol. 60, 1046–1054; Bian et al. (2012) J. Mol. Med. 90, 895–910; Wang et al. (2013) Exp. Neurol. 247, 506–516; Yan et al. (2011) Cardiovasc. Res. 92, 85–94]. However, the regulatory functions of mindin in neointima formation remain unclear. In the present study, mindin expression was significantly down-regulated in platelet-derived growth factor-BB (PDGF-BB)-stimulated vascular smooth muscle cells (VSMCs) and wire injury-stimulated vascular tissue. Using a gain-of-function approach, overexpression of mindin in VSMCs exhibited strong anti-proliferative and anti-migratory effects on VSMCs, whereas significant suppression of intimal hyperplasia was observed in transgenic (TG) mice expressing mindin specifically in smooth muscle cells (SMCs). These mice exhibited blunted VSMC proliferation, migration and phenotypic switching. Conversely, deletion of mindin dramatically exacerbated neointima formation in a wire-injury mouse model, which was further confirmed in a balloon injury-induced vascular lesion model using a novel mindin-KO (knockout) rat strain. From a mechanistic standpoint, the AKT (Protein Kinase B)−GSK3β (glycogen synthase kinase 3β)/mTOR (mammalian target of rapamycin)−FOXO3A (forkhead box O)–FOXO1 signalling axis is responsible for the regulation of mindin during intimal thickening. Interestingly, an AKT inhibitor largely reversed mindin-KO-induced aggravated hyperplasia, suggesting that mindin-mediated neointima formation is AKT-dependent. Taken together, our findings demonstrate that mindin protects against vascular hyperplasia by suppression of abnormal VSMC proliferation, migration and phenotypic switching in an AKT-dependent manner. Up-regulation of mindin might represent an effective therapy for vascular-remodelling-related diseases.

Published
2015

29. Abstract P235: Balancing Truss Expression Paves a Way for Cardiac Hypertrophy Therapy

Author

Xiao-Jing Zhang, Hongliang Li, and Ke-Qiong Deng

Subjects
Pressure overload, medicine.medical_specialty, Cardiac fibrosis, business.industry, Regulator, Stimulation, medicine.disease, Sudden death, Muscle hypertrophy, Endocrinology, Fibrosis, Internal medicine, Internal Medicine, medicine, medicine.symptom, Myopathy, business
Abstract

Pathological cardiac hypertrophy, which is always accompanied by cardiac fibrosis and the resultant cardiac dysfunction, leads to hear failure and even sudden death. The TNF-receptor ubiquitous signaling and scaffolding protein (TRUSS) that is enriched in the heart has been identified as a negative regulator of cancer. However, the role of TRUSS in cardiac remodeling is unknown. Here, we aimed to investigate the potential participation of TRUSS in cardiac hypertrophy and the molecular events by which TRUSS regulates this pathological condition. The pathological cardiac hypertrophy model was established by pressure overload in vivo and Ang II stimulation in vitro . We observed that the expression level of TRUSS was dramatically increased in the heart and in primary cardiomyocytes upon pro-hypertrophic stimuli. To illustrate the functional role of TRUSS in cardiac remodeling, the cardiac specific knockout (KO) or transgenic (TG) mice were employed. After aortic binding (AB) for 4 weeks, TRUSS deficiency conferred significant resistance to pressure overload via significantly inhibiting cardiomyocytes enlargement and fibrosis formation by about 37% and 46%, respectively, whereas dramatically exacerbated hypertrophy, fibrosis, and cardiac dysfunction were shown in TRUSS-TG mice compared to their littermate controls. Mechanistically, TRUSS can directly bind to JNK, a well-known pro-hypertrophic factor, and activate its downstream pathway. Further investigations indicated that the aggravated effect of TRUSS on cardiac hypertrophy can be almost completely reversed by a specific JNK inhibitor, SP600125, indicating a JNK-dependent manner of TRUSS-regulated cardiac hypertrophy. The directly exacerbated function of TRUSS in cardiomyocytes and the JNK-dependent mechanisms were further validated in primary cardiomyocytes that treated with Ang II after infection with AdshTRUSS or AdTRUSS. Notably, the increased protein and mRNA expression of TRUSS was also observed in heart samples from patients with hypertrophic cardiac myopathy. In conclusion, TRUSS functions as a positive regulator of pathological cardiac hypertrophy, suggesting a promising therapeutic approach for the hypertrophy related heart diseases by balancing TRUSS expression.

Published
2016

30. Abstract P234: CTMP Negatively Regulates Pathological Cardiac Hypertrophy via Akt-dependent Manner

Author

Hongliang Li, Xiao-Jing Zhang, and Ke-Qiong Deng

Subjects
Pressure overload, medicine.medical_specialty, business.industry, Regulator, Stimulation, medicine.disease, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Heart failure, Renin–angiotensin system, Internal Medicine, medicine, LY294002, Signal transduction, business, Protein kinase B
Abstract

Pathological cardiac hypertrophy which represents a leading cause of morbidity and mortality worldwide is a pathological process related to multifactorial and multiple molecules and regulated by numerous signaling pathways. Deregulation of AKT signaling is important in cardiac hypertrophy and cardiac dysfunction, but the underlying mechanism is not fully understood. In this study, we identified carboxy-terminal modulator protein (CTMP), an endogenous AKT inhibitor, as a key regulator of cardiac hypertrophy in response to pressure overload. Our results demonstrated that CTMP levels were downregulated by about 40% in aortic banding (AB)–induced hypertrophied mice hearts and 50% in failing human hearts compared to their controls respectively. Mice overexpressing CTMP specifically in the heart were resistant to AB-induced cardiac hypertrophy, whereas cardiac-specific conditional CTMP-knockout mice exhibited an aggravated phenotype induced by pressure overload. Additionally, gain-or-loss of function experiments mediated by adenovirus demonstrated that CTMP also prevented an angiotensin II–induced hypertrophic response in isolated cardiomyocytes in vitro . Mechanistically, we discovered that AKT signaling was significantly activated in AB-treated WT hearts, which was blocked by cardiac overexpression of CTMP, whereas being enhanced by loss of CTMP in response to chronic pressure overload and agonist stimulation. Moreover, rescue-experiments revealed that inhibition of AKT activation through LY294002 ameliorated the cardiac abnormalities in CTMP-knockout mice after AB. Taken together, our present study provides both in vitro and in vivo evidences that CTMP functions as a novel negative regulator factor of pathological cardiac hypertrophy. The underlying mechanisms responsible for CTMP-elicited effects are dependent on the inhibition of AKT signaling. The above-mentioned findings also expand our knowledge of the mechanisms of cardiac hypertrophy and provide potential therapeutic targets for pathological cardiac hypertrophy and heart failure.

Published
2016

31. Suppressor of IKKɛ is an essential negative regulator of pathological cardiac hypertrophy

Author

Xueyong Zhu, Xi Jiang, Lingchen Gao, Yichao Zhao, Xiang Wei, Xue-Hai Zhu, Hongliang Li, Yan-Xiao Ji, Xiao-Jing Zhang, Peng Zhang, Qinglin Yang, Jing Fang, Ke-Qiong Deng, Aibing Wang, Jun Pu, Lu Gao, and Yan Zhang

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, Science, Transgene, Down-Regulation, General Physics and Astronomy, Cardiomegaly, Mice, Transgenic, Protein Serine-Threonine Kinases, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, TANK-binding kinase 1, Downregulation and upregulation, Internal medicine, medicine, Animals, Humans, Myocyte, Myocytes, Cardiac, Protein kinase B, Mice, Knockout, Multidisciplinary, Intracellular Signaling Peptides and Proteins, General Chemistry, medicine.disease, Hedgehog signaling pathway, Rats, Mice, Inbred C57BL, Disease Models, Animal, Macaca fascicularis, 030104 developmental biology, Endocrinology, Heart failure, Cancer research, Female, Signal transduction, Protein Binding, Signal Transduction
Abstract

Although pathological cardiac hypertrophy represents a leading cause of morbidity and mortality worldwide, our understanding of the molecular mechanisms underlying this disease is still poor. Here, we demonstrate that suppressor of IKKɛ (SIKE), a negative regulator of the interferon pathway, attenuates pathological cardiac hypertrophy in rodents and non-human primates in a TANK-binding kinase 1 (TBK1)/AKT-dependent manner. Sike-deficient mice develop cardiac hypertrophy and heart failure, whereas Sike-overexpressing transgenic (Sike-TG) mice are protected from hypertrophic stimuli. Mechanistically, SIKE directly interacts with TBK1 to inhibit the TBK1-AKT signalling pathway, thereby achieving its anti-hypertrophic action. The suppression of cardiac remodelling by SIKE is further validated in rats and monkeys. Collectively, these findings identify SIKE as a negative regulator of cardiac remodelling in multiple animal species due to its inhibitory regulation of the TBK1/AKT axis, suggesting that SIKE may represent a therapeutic target for the treatment of cardiac hypertrophy and heart failure., Identifying pathways that cause pathological cardiac hypertrophy holds great therapeutic potential. Here the authors discover one such pathway and show that SIKE, an inhibitor of interferon signalling, prevents pathological but not physiological cardiac hypertrophy by interacting with TBK1 and modulating the TBK1/AKT signalling in rodents and monkeys.

Published
2016

32. The long noncoding RNA Chaer defines an epigenetic checkpoint in cardiac hypertrophy

Author

Yen-Sin Ang, Huang-Tian Yang, Yan-Xiao Ji, Shuxun Ren, Shen Li, Arjun Deb, Jun Gong, Tomohiro Yokota, Ke-Qiong Deng, Chen Gao, Yibin Wang, Xiao-Jing Zhang, Xinshu Xiao, He Wang, Thomas M. Vondriska, Hongliang Li, Peng Zhang, Deepak Srivastava, Xinghua Wang, Zhihua Wang, Guangping Li, Ashley A. Cass, and Iris Chen

Subjects
0301 basic medicine, Chromatin Immunoprecipitation, Heart growth, Immunoblotting, Induced Pluripotent Stem Cells, Regulator, Cardiomegaly, macromolecular substances, In Vitro Techniques, Mechanistic Target of Rapamycin Complex 1, Real-Time Polymerase Chain Reaction, Methylation, General Biochemistry, Genetics and Molecular Biology, Article, Epigenesis, Genetic, 03 medical and health sciences, Mice, Gene Knockdown Techniques, Animals, Humans, Computer Simulation, Myocytes, Cardiac, Epigenetics, In Situ Hybridization, Fluorescence, Genetics, Mice, Knockout, biology, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Myocardium, TOR Serine-Threonine Kinases, Polycomb Repressive Complex 2, RNA, Heart, General Medicine, Blotting, Northern, Long non-coding RNA, Cell biology, Rats, Histone Code, 030104 developmental biology, Echocardiography, Multiprotein Complexes, biology.protein, RNA, Long Noncoding, PRC2, Chromatin immunoprecipitation
Abstract

Epigenetic reprogramming is a critical process of pathological gene induction during cardiac hypertrophy and remodeling, but the underlying regulatory mechanisms remain to be elucidated. Here we identified a heart-enriched long noncoding (lnc)RNA, named cardiac-hypertrophy-associated epigenetic regulator (Chaer), which is necessary for the development of cardiac hypertrophy. Mechanistically, Chaer directly interacts with the catalytic subunit of polycomb repressor complex 2 (PRC2). This interaction, which is mediated by a 66-mer motif in Chaer, interferes with PRC2 targeting to genomic loci, thereby inhibiting histone H3 lysine 27 methylation at the promoter regions of genes involved in cardiac hypertrophy. The interaction between Chaer and PRC2 is transiently induced after hormone or stress stimulation in a process involving mammalian target of rapamycin complex 1, and this interaction is a prerequisite for epigenetic reprogramming and induction of genes involved in hypertrophy. Inhibition of Chaer expression in the heart before, but not after, the onset of pressure overload substantially attenuates cardiac hypertrophy and dysfunction. Our study reveals that stress-induced pathological gene activation in the heart requires a previously uncharacterized lncRNA-dependent epigenetic checkpoint.

Published
2016

33. Targeting Transmembrane BAX Inhibitor Motif Containing 1 Alleviates Pathological Cardiac Hypertrophy.

Author

Ke-Qiong Deng, Guang-Nian Zhao, Zhihua Wang, Jing Fang, Zhou Jiang, Jun Gong, Feng-Juan Yan, Xue-Yong Zhu, Peng Zhang, Zhi-Gang She, Hongliang Li, Deng, Ke-Qiong, Zhao, Guang-Nian, Wang, Zhihua, Fang, Jing, Jiang, Zhou, Gong, Jun, Yan, Feng-Juan, Zhu, Xue-Yong, and Zhang, Peng

Subjects
*CARDIAC hypertrophy, *HEART failure, *MORTALITY, *BAX protein, *PROTEOLYSIS, *LYSOSOMAL storage diseases, *GENETIC overexpression, *CELL metabolism, *HEART metabolism, *PROTEIN metabolism, *AMINO acids, *ANIMAL experimentation, *BIOLOGICAL models, *CELL receptors, *CELLS, *CELLULAR signal transduction, *COMPARATIVE studies, *LYSOSOMES, *RESEARCH methodology, *MEDICAL cooperation, *MEMBRANE proteins, *MICE, *MYOCARDIUM, *PRIMATES, *PROTEINS, *RATS, *RESEARCH, *TRANSCRIPTION factors, *DNA-binding proteins, *EVALUATION research
Abstract

Background: Cardiac hypertrophy and its resultant heart failure are among the most common causes of mortality worldwide. Abnormal protein degradation, especially the impaired lysosomal degradation of large organelles and membrane proteins, is involved in the progression of cardiac hypertrophy. However, the underlying mechanisms have not been fully elucidated.Methods: We investigated cardiac transmembrane BAX inhibitor motif containing 1 (TMBIM1) mRNA and protein expression levels in samples from patients with heart failure and mice with aortic banding (AB)-induced cardiac hypertrophy. We generated cardiac-specific Tmbim1 knockout mice and cardiac-specific Tmbim1-overexpressing transgenic mice and then challenged them with AB surgery. We used microarray, confocal image, and coimmunoprecipitation analyses to identify the downstream targets of TMBIM1 in cardiac hypertrophy. Tmbim1/Tlr4 double-knockout mice were generated to investigate whether the effects of TMBIM1 on cardiac hypertrophy were Toll-like receptor 4 (TLR4) dependent. Finally, lentivirus-mediated TMBIM1 overexpression in a monkey AB model was performed to evaluate the therapeutic potential of TMBIM1.Results: TMBIM1 expression was significantly downregulated on hypertrophic stimuli in both human and mice heart samples. Silencing cardiac Tmbim1 aggravated AB-induced cardiac hypertrophy. This effect was blunted by Tmbim1 overexpression. Transcriptome profiling revealed that the TLR4 signaling pathway was disrupted dramatically by manipulation of Tmbim1. The effects of TMBIM1 on cardiac hypertrophy were shown to be dependent on TLR4 in double-knockout mice. Fluorescent staining indicated that TMBIM1 promoted the lysosome-mediated degradation of activated TLR4. Coimmunoprecipitation assays confirmed that TMBIM1 directly interacted with tumor susceptibility gene 101 via a PTAP motif and accelerated the formation of multivesicular bodies that delivered TLR4 to the lysosomes. Finally, lentivirus-mediated TMBIM1 overexpression reversed AB-induced cardiac hypertrophy in monkeys.Conclusions: TMBIM1 protects against pathological cardiac hypertrophy through promoting the lysosomal degradation of activated TLR4. Our findings reveal the central role of TMBIM1 as a multivesicular body regulator in the progression of pathological cardiac hypertrophy, as well as the role of vesicle trafficking in signaling regulation during cardiac hypertrophy. Moreover, targeting TMBIM1 could be a novel therapeutic strategy for treating cardiac hypertrophy and heart failure. [ABSTRACT FROM AUTHOR]

Published
2018
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34. Restoration of Circulating MFGE8 (Milk Fat Globule-EGF Factor 8) Attenuates Cardiac Hypertrophy Through Inhibition of Akt Pathway.

Author

Ke-Qiong Deng, Jing Li, Zhi-Gang She, Jun Gong, Wen-Lin Cheng, Fu-Han Gong, Xue-Yong Zhu, Yan Zhang, Zhihua Wang, Hongliang Li, Deng, Ke-Qiong, Li, Jing, She, Zhi-Gang, Gong, Jun, Cheng, Wen-Lin, Gong, Fu-Han, Zhu, Xue-Yong, Zhang, Yan, Wang, Zhihua, and Li, Hongliang

Abstract

Cardiac hypertrophy occurs in response to numerous stimuli like neurohumoral stress, pressure overload, infection, and injury, and leads to heart failure. Mfge8 (milk fat globule-EGF factor 8) is a secreted protein involved in various human diseases, but its regulation and function during cardiac hypertrophy remain unexplored. Here, we found that circulating MFGE8 levels declined significantly in failing hearts from patients with dilated cardiomyopathy. Correlation analyses revealed that circulating MFGE8 levels were negatively correlated with the severity of cardiac dysfunction and remodeling in affected patients. Deleting Mfge8 in mice maintained normal heart function at basal level but substantially exacerbated the hypertrophic enlargement of cardiomyocytes, reprogramming of pathological genes, contractile dysfunction, and myocardial fibrosis after aortic banding surgery. In contrast, cardiac-specific Mfge8 overexpression in transgenic mice significantly blunted aortic banding-induced cardiac hypertrophy. Whereas MAPK (mitogen-activated protein kinase) pathways were unaffected in either Mfge8-knockout or Mfge8-overexpressing mice, the activated Akt/PKB (protein kinase B)-Gsk-3β (glycogen synthase kinase-3β)/mTOR (mammalian target of rapamycin) pathway after aortic banding was significantly potentiated by Mfge8 deficiency but suppressed by Mfge8 overexpression. Inhibition of Akt with MK-2206 blocked the prohypertrophic effects of Mfge8 deficiency in angiotensin II-treated neonatal rat cardiomyocytes. Finally, administering a recombinant human MFGE8 in mice in vivo alleviated cardiac hypertrophy induced by aortic banding. Our findings indicate that Mfge8 is an endogenous negative regulator of pathological cardiac hypertrophy and may, thus, have potential both as a novel biomarker and as a therapeutic target for treatment of cardiac hypertrophy. [ABSTRACT FROM AUTHOR]

Published
2017
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35. Control of Pathological Cardiac Hypertrophy by Transcriptional Corepressor IRF2BP2 (Interferon Regulatory Factor-2 Binding Protein 2).

Author

Jing Fang, Tianyu Li, Xuehai Zhu, Ke-Qiong Deng, Yan-Xiao Ji, Chun Fang, Xiao-Jing Zhang, Jun-Hong Guo, Peng Zhang, Hongliang Li, Xiang Wei, Fang, Jing, Li, Tianyu, Zhu, Xuehai, Deng, Ke-Qiong, Ji, Yan-Xiao, Fang, Chun, Zhang, Xiao-Jing, Guo, Jun-Hong, and Zhang, Peng

Abstract

The transcription factor NFAT1 (nuclear factor of activated T-cells 1), with the aid of transcriptional coactivators, has been recognized for its necessity and sufficiency to drive pathological cardiac hypertrophy. However, how the transcriptional activity of NFAT1 in terms of cardiac hypertrophy is controlled at the transcriptional level has not been well defined. Herein, we showed that a cardiac-enriched protein IRF2BP2 (interferon regulatory factor-2 binding protein 2) was further upregulated in both human and mouse hypertrophied myocardium and negatively regulated cardiomyocyte hypertrophic response in vitro. By generating cardiomyocyte-specific Irf2bp2 knockout and Irf2bp2-transgenic mouse strains, our in vivo experiments showed that, whereas IRF2BP2 loss-of-function exacerbated both aortic banding- and angiotensin II infusion-induced cardiac hypertrophic response, IRF2BP2 overexpression exerted a strong protective effect against these maladaptive processes. Particularly, IRF2BP2 directly interacted with the C-terminal transactivation domain of NFAT1 by competing with myocyte enhancer factor-2C and disturbing their transcriptional synergism, thereby impeding NFAT1-transactivated hypertrophic transcriptome. As a result, the devastating effect of Irf2bp2 deficiency on cardiac hypertrophy was largely rescued by NFAT1 blockage. Our study, thus, defined IRF2BP2 as a novel negative regulator in controlling pathological cardiac hypertrophy at the transcriptional level. [ABSTRACT FROM AUTHOR]

Published
2017
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36. Tripartite Motif 8 Contributes to Pathological Cardiac Hypertrophy Through Enhancing Transforming Growth Factor β-Activated Kinase 1-Dependent Signaling Pathways.

Author

Lijuan Chen, Jia Huang, Yan-xiao Ji, Fanghua Mei, Pi-xiao Wang, Ke-qiong Deng, Xi Jiang, Genshan Ma, Hongliang Li, Chen, Lijuan, Huang, Jia, Ji, Yan-Xiao, Mei, Fanghua, Wang, Pi-Xiao, Deng, Ke-Qiong, Jiang, Xi, Ma, Genshan, and Li, Hongliang

Abstract

Tripartite motif (TRIM) 8 functions as an E3 ubiquitin ligase, interacting with and ubiquitinating diverse substrates, and is implicated in various pathological processes. However, the function of TRIM8 in the heart remains largely uncharacterized. This study aims to explore the role of TRIM8 in the development of pathological cardiac hypertrophy. Mice and isolated neonatal rat cardiomyocytes overexpressing or lacking TRIM8 were examined in several experiments. The effect of aortic banding-induced cardiac hypertrophy was analyzed by echocardiographic, pathological and molecular analyses. Our results indicated that the TRIM8 overexpression in hearts exacerbated the cardiac hypertrophy triggered by aortic banding. In contrast, the development of pathological cardiac hypertrophy was profoundly blocked in TRIM8-deficient hearts. Mechanistically, our study suggests that TRIM8 may elicit cardiodetrimental effects by promoting the activation of transforming growth factor β-activated kinase 1 (TAK1)-p38/JNK signaling pathways. Similar results were observed in cultured neonatal rat cardiomyocytes treated with angiotensin II. The rescue experiments using the TAK1-specific inhibitor 5z-7-ox confirmed the requirement of TAK1 activation in TRIM8-mediated pathological cardiac hypertrophy. Furthermore, TRIM8 contributed to TAK1 activation by binding to and promoting TAK1 ubiquitination. In conclusion, our study demonstrates that TRIM8 plays a deleterious role in pressure overload-induced cardiac hypertrophy by accelerating the activation of TAK1-dependent signaling pathways. [ABSTRACT FROM AUTHOR]

Published
2017
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