Your search keyword '"Coxsackievirus Infections genetics"' showing total 212 results

1. The Type 1 Diabetes-Associated Single Nucleotide Polymorphism rs1990760 in IFIH1 Is Associated with Increased Basal Type I IFNs and IFN-stimulated Gene Expression.

Author

Taylor JP, Blum SI, Graffeo HC, Shang Q, Qiu S, Green TJ, Botta D, Lund FE, and Tse HM

Subjects

Humans, Enterovirus B, Human physiology, Genetic Predisposition to Disease, Coxsackievirus Infections immunology, Coxsackievirus Infections genetics, Gene Expression Regulation, Signal Transduction immunology, Signal Transduction genetics, Polymorphism, Single Nucleotide, Interferon-Induced Helicase, IFIH1 genetics, Diabetes Mellitus, Type 1 genetics, Diabetes Mellitus, Type 1 immunology, Interferon Type I genetics

Abstract

Type 1 diabetes (T1D) is a chronic autoimmune disease that is caused by a combination of genetic and environmental risk factors. In this study, we sought to determine whether a known genetic risk factor, the rs1990760 single nucleotide polymorphism (SNP) (A946T) in IFIH1, resulted in a gain of function in the MDA5 protein and the effects of this mutation on the regulation of type I IFNs during infection with the diabetogenic virus coxsackievirus B3. We found that in cell lines overexpressing the risk variant IFIH1946T there was an elevated level of basal type I IFN signaling and increased basal IFN-stimulated gene expression. An investigation into the mechanism demonstrated that recombinant MDA5 with the A946T mutation had increased ATPase activity in vitro. We also assessed the effect of this SNP in primary human PBMCs from healthy donors to determine whether this SNP influenced their response to infection with coxsackievirus B3. However, we observed no significant changes in type I IFN expression or downstream induction of IFN-stimulated genes in PBMCs from donors carrying the risk allele IFIH1946T. These findings demonstrate the need for a deeper understanding of how mutations in T1D-associated genes contribute to disease onset in specific cellular contexts., (Copyright © 2024 by The American Association of Immunologists, Inc.)

Published

2024

2. LncRNA XIST knockdown reduces myocardial damage in myocarditis by targeting the miR-140-3p/RIPK1 axis.

Author

Zhang Z, Zhu D, Shi P, Wu J, Li F, and Chen Y

Subjects

Humans, Cell Line, Rats, Animals, Myocytes, Cardiac metabolism, Myocytes, Cardiac pathology, Enterovirus B, Human, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Gene Knockdown Techniques, Oxidative Stress, Myocardium metabolism, Myocardium pathology, RNA, Long Noncoding genetics, RNA, Long Noncoding metabolism, MicroRNAs genetics, MicroRNAs metabolism, Myocarditis metabolism, Myocarditis genetics, Myocarditis pathology, Apoptosis, Receptor-Interacting Protein Serine-Threonine Kinases metabolism, Receptor-Interacting Protein Serine-Threonine Kinases genetics

Abstract

Viral myocarditis (MC) is caused by Coxsackie virus B3 (CVB3)-induced cardiomyocyte apoptosis and inflammation, and changes in miRNA and lncRNA are linked to cardiac remodeling. The long non-coding RNA XIST (XIST) has been identified as a regulator in various pathological processes in heart diseases, but its role in CVB3-induced MC is not well understood. This research aimed to evaluate the impact that XIST has on CVB3-induced MC as well as the mechanism behind this effect. XIST expression in CVB3-exposed H9c2 cells (H9c2 cells) was evaluated by qRT-PCR. In CVB3-exposed H9c2 cells, reactive oxygen species production, inflammatory mediators, and apoptosis were experimentally observed. An investigation into and confirmation of the existence of an interaction involving XIST, miR-140-3p, and RIPK1 were carried out. The findings showed that CVB3 induced upregulation of XIST in H9c2 cells. However, XIST knockdown reduced oxidative stress, inflammation, and apoptosis of CVB3-exposed H9c2 cells. XIST was specifically bound to miR-140-3p, and there was mutual negative regulation between the two. Moreover, XIST downregulated RIPK1, which was mediated by miR-140-3p. The study suggests that downregulating XIST can alleviate inflammatory injury in CVB3-exposed H9c2 cells through the miR-140-3p/RIPK1 axis. These findings provide novel insights into the underlying mechanisms of MC.

Published

2024

3. Sex Differences in Expression of Pro-Inflammatory Markers and miRNAs in a Mouse Model of CVB3 Myocarditis.

Author

Estepa M, Niehues MH, Vakhrusheva O, Haritonow N, Ladilov Y, Barcena ML, and Regitz-Zagrosek V

Subjects

Animals, Female, Male, Mice, Enterovirus B, Human, Biomarkers metabolism, Sex Characteristics, Cytokines metabolism, Cytokines genetics, Myocardium metabolism, Myocardium pathology, Inflammation genetics, Inflammation metabolism, Sex Factors, Gene Expression Regulation, Myocarditis metabolism, Myocarditis virology, Myocarditis genetics, MicroRNAs genetics, MicroRNAs metabolism, Disease Models, Animal, Coxsackievirus Infections metabolism, Coxsackievirus Infections genetics, Coxsackievirus Infections virology

Abstract

Myocarditis is an inflammatory disease that may lead to dilated cardiomyopathy. Viral infection of the myocardium triggers immune responses, which involve, among others, macrophage infiltration, oxidative stress, expression of pro-inflammatory cytokines, and microRNAs (miRNAs). The cardioprotective role of estrogen in myocarditis is well documented; however, sex differences in the miRNA expression in chronic myocarditis are still poorly understood, and studying them further was the aim of the present study. Male and female ABY/SnJ mice were infected with CVB3. Twenty-eight days later, cardiac tissue from both infected and control mice was used for real-time PCR and Western blot analysis. NFκB, IL-6, iNOS, TNF-α, IL-1β, MCP-1, c-fos, and osteopontin (OPN) were used to examine the inflammatory state in the heart. Furthermore, the expression of several inflammation- and remodeling-related miRNAs was analyzed. NFκB, IL-6, TNF-α, IL-1β, iNOS, and MCP-1 were significantly upregulated in male mice with CVB3-induced chronic myocarditis, whereas OPN mRNA expression was increased only in females. Further analysis revealed downregulation of some anti-inflammatory miRNA in male hearts (let7a), with upregulation in female hearts (let7b). In addition, dysregulation of remodeling-related miRNAs (miR27b and mir199a) in a sex-dependent manner was observed. Taken together, the results of the present study suggest a sex-specific expression of pro-inflammatory markers as well as inflammation- and remodeling-related miRNAs, with a higher pro-inflammatory response in male CVB3 myocarditis mice.

Published

2024

4. LncRNA MALAT1 to Enhance Pyroptosis in Viral Myocarditis Through UPF1-Mediated SIRT6 mRNA Decay and Wnt-β-Catenin Signal Pathway.

Author

Zeng M, Chen Z, Wang Y, Yang Z, Xiang J, Wang X, and Wang X

Subjects

Animals, Male, Enterovirus B, Human pathogenicity, Cell Line, Trans-Activators genetics, Trans-Activators metabolism, RNA Helicases metabolism, RNA Helicases genetics, Mice, beta Catenin, RNA, Long Noncoding genetics, RNA, Long Noncoding metabolism, Myocarditis virology, Myocarditis pathology, Myocarditis metabolism, Myocarditis genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Coxsackievirus Infections genetics, Coxsackievirus Infections pathology, Pyroptosis, Disease Models, Animal, RNA Stability, Sirtuins metabolism, Sirtuins genetics, Mice, Inbred BALB C, Wnt Signaling Pathway, Myocytes, Cardiac virology, Myocytes, Cardiac pathology, Myocytes, Cardiac metabolism, Myocytes, Cardiac enzymology

Abstract

Viral myocarditis (VMC) is an inflammatory disease of the myocardium caused by cardioviral infection, especially coxsackievirus B3 (CVB3), and is a major contributor to acute heart failure and sudden cardiac death in children and adolescents. LncRNA MALAT1 knockdown reportedly inhibits the differentiation of Th17 cells to attenuate CVB3-induced VMC in mice. Moreover, long non-coding RNAs (lncRNAs) interact with RNA-binding proteins (RBPs) to regulate UPF1-mediated mRNA decay. However, it remains unclear whether MALAT1 can bind to UPF1 to mediate the mRNA decay of its target genes in VMC. Herein, we aimed to explore the effect of lncRNA MALAT1 on UPF1-mediated SIRT6 mRNA decay in VMC using in vivo and in vitro experiments. CVB3-infected BABL/C mice were used as VMC models, and MALAT1 interfering adenovirus was injected to achieve MALAT1 knockdown. The heart function of the VMC mice was assessed using echocardiography. Pathological changes in myocardial tissues were assessed after hematoxylin-eosin staining. Myocardial injury and inflammation were evaluated by measuring creatine kinase isoenzyme B, cardiac troponin T, interleukin (IL)-1β, and IL-18. TUNEL staining was performed to assess apoptosis in myocardial tissues. In vitro experiments were performed using H9c2 cells after transfection and CVB3 infection. The lactic dehydrogenase release, caspase-1 activity, and IL-1β and IL-18 levels in the cellular supernatant were detected. Western blotting was performed to determine the expression of pyroptosis-related proteins (GSDMD-N, NLRP3, ASC, and Cleaved-Caspase-1) and Wnt/β-catenin signal pathway-related proteins (Wnt1, β-catenin, and p-GSK-3β). RNA immunoprecipitation and RNA stability assays assessed the relationship between MALAT1, UPF1, and SIRT6. CVB3-infected mice and H9c2 cells exhibited elevated MALAT1 and reduced SIRT6 expression. MALAT1 knockdown or SIRT6 overexpression suppressed inflammation and pyroptosis and inhibited the activation of the Wnt/β-catenin signal pathway in myocardial tissues and cells. MALAT1 enhanced the enrichment of SIRT6 mRNA by UPF1 and disturbed the stability of SIRT6 mRNA to promote the development of VMC. MALAT1 can bind UPF1 to mediate SIRT6 mRNA decay and activate the Wnt/β-catenin signal pathway in VMC., Competing Interests: Declarations Conflict of interest The authors declare that they have no competing interests. Ethical Approval and Consent to Participate The experimental design was approved by the Ethics Committee of Hunan Children’s Hospital (Approval no. KYSQ-2022–304). All experiments involving mice were conducted based on the instructions on the Guide for Care and Use of Laboratory Animals issued by the National Institutes of Health. Consent for Publication Not applicable., (© 2024. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

5. Analysis of miRNAs involved in mouse brain injury upon Coxsackievirus A6 infection.

Author

Sun Y, Hao Y, Wu J, Qian S, Shen S, and Yu Y

Subjects

Animals, Mice, Brain virology, Brain pathology, Brain metabolism, Coxsackievirus Infections virology, Coxsackievirus Infections genetics, Brain Injuries virology, Brain Injuries genetics, Gene Expression Profiling, Enterovirus A, Human genetics, Enterovirus A, Human pathogenicity, Enterovirus genetics, Enterovirus pathogenicity, Hand, Foot and Mouth Disease virology, MicroRNAs genetics, MicroRNAs metabolism, Disease Models, Animal

Abstract

Introduction: Coxsackievirus A6 (CV-A6) has emerged as the predominant epidemic strain responsible for hand, foot and mouth disease (HFMD). CV-A6 infection can result in severe clinical manifestations, including encephalitis, meningitis, and potentially life-threatening central nervous system disorders. Our previous research findings demonstrated that neonatal mice infected with CV-A6 exhibited limb weakness, paralysis, and ultimately succumbed to death. However, the underlying mechanism of CV-A6-induced nervous system injury remains elusive. Numerous reports have highlighted the pivotal role of miRNAs in various viral infections., Methods: Separately established infection and control groups of mice were used to create miRNA profiles of the brain tissues before and after CV-A6 transfection, followed by experimental verification, prediction, and analysis of the results., Results: At 2 days post-infection (dpi), 4 dpi, and 2dpi vs 4dpi, we identified 175, 198 and 78 significantly differentially expressed miRNAs respectively using qRT-PCR for validation purposes. Subsequently, we predicted target genes of these differentially expressed miRNAs and determined their potential targets through GO (Gene Ontology) enrichment analysis and KEGG (Kyoto Encyclopedia of Genes and Genomes) enrichment analysis. Finally, we verified the miRNA-mRNA pairing via double luciferase experiments while confirming functional enrichment of target genes through Western Blotting analyses., Discussion: The results from this study suggest that transcriptional regulation, neuronal necrosis, pro-inflammatory cytokine release, and antiviral immunity are all implicated in the pathogenesis of central nervous system injury in mice infected with CV-A6. Brain injury resulting from CV-A6 infection may involve multiple pathways, including glial cell activation, neuronal necrosis, synaptic destruction, degenerative diseases of the nervous system. It can even encompass destruction of the blood-brain barrier, leading to central nervous system injury. The dysregulated miRNAs and signaling pathways discovered in this study provide valuable insights for further investigations into the pathogenesis of CV-A6., Competing Interests: Authors YS, JW, SQ, and SS were employed by the company Wuhan Institute of Biological Products Co. Ltd. The remaining author declares that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Sun, Hao, Wu, Qian, Shen and Yu.)

Published

2024

6. STAT3 Increases CVB3 Replication and Acute Pancreatitis and Myocarditis Pathology via Impeding Nuclear Translocation of STAT1 and Interferon-Stimulated Gene Expression.

Author

Liang T, Zhang Z, Bai Z, Xu L, and Xu W

Subjects

Animals, Mice, Humans, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Coxsackievirus Infections pathology, Coxsackievirus Infections genetics, Cell Nucleus metabolism, Male, Active Transport, Cell Nucleus, Gene Expression Regulation, Acute Disease, Cell Line, Signal Transduction, STAT1 Transcription Factor metabolism, STAT1 Transcription Factor genetics, Myocarditis virology, Myocarditis metabolism, Myocarditis pathology, Myocarditis genetics, STAT3 Transcription Factor metabolism, STAT3 Transcription Factor genetics, Pancreatitis metabolism, Pancreatitis virology, Pancreatitis pathology, Pancreatitis genetics, Enterovirus B, Human physiology, Virus Replication

Abstract

Acute pancreatitis (AP) is an inflammatory disease initiated by the death of exocrine acinar cells, but its pathogenesis remains unclear. Signal transducer and activator of transcription 3 (STAT3) is a multifunctional factor that regulates immunity and the inflammatory response. The protective role of STAT3 is reported in Coxsackievirus B3 (CVB3)-induced cardiac fibrosis, yet the exact role of STAT3 in modulating viral-induced STAT1 activation and type I interferon (IFN)-stimulated gene (ISG) transcription in the pancreas remains unclarified. In this study, we tested whether STAT3 regulated viral-induced STAT1 translocation. We found that CVB3, particularly capsid VP1 protein, markedly upregulated the phosphorylation and nuclear import of STAT3 (p-STAT3) while it significantly impeded the nuclear translocation of p-STAT1 in the pancreases and hearts of mice on day 3 postinfection (p.i.). Immunoblotting and an immunofluorescent assay demonstrated the increased expression and nuclear translocation of p-STAT3 but a blunted p-STAT1 nuclear translocation in CVB3-infected acinar 266-6 cells. STAT3 shRNA knockdown or STAT3 inhibitors reduced viral replication via the rescue of STAT1 nuclear translocation and increasing the ISRE activity and ISG transcription in vitro. The knockdown of STAT1 blocked the antiviral effect of the STAT3 inhibitor. STAT3 inhibits STAT1 activation by virally inducing a potent inhibitor of IFN signaling, the suppressor of cytokine signaling-3 ((SOCS)-3). Sustained pSTAT1 and the elevated expression of ISGs were induced in SOCS3 knockdown cells. The in vivo administration of HJC0152, a pharmaceutical STAT3 inhibitor, mitigated the viral-induced AP and myocarditis pathology via increasing the IFNβ as well as ISG expression on day 3 p.i. and reducing the viral load in multi-organs. These findings define STAT3 as a negative regulator of the type I IFN response via impeding the nuclear STAT1 translocation that otherwise triggers ISG induction in infected pancreases and hearts. Our findings identify STAT3 as an antagonizing factor of the IFN-STAT1 signaling pathway and provide a potential therapeutic target for viral-induced AP and myocarditis.

Published

2024

7. Acetylation of FOXO1 activates Bim expression involved in CVB3 induced cardiomyocyte apoptosis.

Author

Hu Y, Yi L, Yang Y, Wu Z, Kong M, Kang Z, and Yang Z

Subjects

Animals, Acetylation, Humans, Male, Mice, Signal Transduction, Rats, Bcl-2-Like Protein 11 metabolism, Bcl-2-Like Protein 11 genetics, Apoptosis genetics, Myocytes, Cardiac virology, Myocytes, Cardiac metabolism, Myocytes, Cardiac pathology, Forkhead Box Protein O1 metabolism, Forkhead Box Protein O1 genetics, Myocarditis virology, Myocarditis metabolism, Myocarditis genetics, Myocarditis pathology, Enterovirus B, Human physiology, Coxsackievirus Infections genetics, Coxsackievirus Infections virology, Coxsackievirus Infections metabolism, Coxsackievirus Infections pathology

Abstract

Viral myocarditis (VMC) is the major reason for sudden cardiac death among both children and young adults. Of these, coxsackievirus B3 (CVB3) is the most common causative agent of myocarditis. Recently, the role of signaling pathways in the pathogenesis of VMC has been evaluated in several studies, which has provided a new perspective on identifying potential therapeutic targets for this hitherto incurable disease. In the present study, in vivo and in vitro experiments showed that CVB3 infection leads to increased Bim expression and triggers apoptosis. In addition, by knocking down Bim using RNAi, we further confirmed the biological function of Bim in apoptosis induced by CVB3 infection. We additionally found that Bim and forkhead box O1 class (FOXO1) inhibition significantly increased the viability of CVB3-infected cells while blocking viral replication and viral release. Moreover, CVB3-induced Bim expression was directly dependent on FOXO1 acetylation, which is catalyzed by the co-regulation of CBP and SirTs. Furthermore, the acetylation of FOXO1 was an important step in Bim activation and apoptosis induced by CVB3 infection. The findings of this study suggest that CVB3 infection induces apoptosis through the FOXO1 acetylation-Bim pathway, thus providing new insights for developing potential therapeutic targets for enteroviral myocarditis., (© 2023. The Author(s).)

Published

2024

8. CaMKIIδ, Stabilized by RNA N6-Methyladenosine Reader IGF2BP2, Boosts Coxsackievirus B3-Induced Myocardial Inflammation via Interacting with TIRAP.

Author

Xiao Q, Liu L, Qian W, Kang T, Ying R, and Nie J

Subjects

Animals, Male, Mice, Adenosine analogs & derivatives, Adenosine metabolism, Cell Proliferation, Cells, Cultured, Enterovirus B, Human pathogenicity, Inflammation Mediators metabolism, Mice, Inbred BALB C, Ventricular Function, Left, Apoptosis, Calcium-Calmodulin-Dependent Protein Kinase Type 2 metabolism, Calcium-Calmodulin-Dependent Protein Kinase Type 2 genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections genetics, Coxsackievirus Infections enzymology, Coxsackievirus Infections virology, Coxsackievirus Infections pathology, Disease Models, Animal, Myocarditis metabolism, Myocarditis genetics, Myocarditis pathology, Myocarditis virology, Myocarditis enzymology, Myocytes, Cardiac enzymology, Myocytes, Cardiac pathology, Myocytes, Cardiac metabolism, Myocytes, Cardiac virology, NF-kappa B metabolism, Receptors, Interleukin-1 metabolism, Receptors, Interleukin-1 genetics, RNA-Binding Proteins metabolism, RNA-Binding Proteins genetics, Signal Transduction

Abstract

Calcium/calmodulin-dependent protein kinase II (CaMKII) has been demonstrated to be aberrantly activated in viral myocarditis (VMC), but the role of its subtype CaMKIIδ in VMC remains unclear.VMC mice and cardiomyocytes models were induced by Coxsackievirus B3 (CVB3) treatment. Mice that underwent sham surgery and saline-treated cardiomyocytes served as controls. Body weight, survival, left ventricular ejection fraction (LVEF), and fractional shortening (LVFS) were measured, and HE staining was performed to evaluate heart function in VMC mice model and sham control. Inflammation factors in serum or cell supernatant were detected by ELISA. Expressions of CaMKIIδ, Toll/interleukin-1 receptor domain containing adaptor protein (TIRAP), insulin-like growth factor 2 mRNA binding protein 2 (IGF2BP2), nuclear factor NF-kappaB (NF-κB) signals, and inflammation factors were examined by quantitative real time polymerase chain reaction (qRT-PCR) or western blot. CCK-8, EdU, and flow cytometry were used to evaluate cell behaviors. Co-immunoprecipitation (Co-IP), RNA immunoprecipitation (RIP), and RNA pull-down were utilized to validate molecule interaction. Methylated RNA immunoprecipitation (MeRIP) was performed to measure N6-methyladenosine (m6A) level of specific molecule.CaMKIIδ was upregulated in VMC mice and CVB3-treated primary cardiomyocytes, of which knockdown improved cell viability, proliferation, and suppressed cell apoptosis in vitro, thereby alleviating myocarditis in vivo. The stability of CaMKIIδ was attributed to the presence of IGF2BP2 through m6A modification. Loss of CaMKIIδ repressed NF-κB pathway via negatively and directly regulating TIRAP to be involved in inflammatory damage.CaMKIIδ, stabilized by m6A reader IGF2BP2, modulated NF-κB pathway via interacting with TIRAP to alter cell viability, proliferation, and apoptosis, thereby affecting VMC outcome., (© 2024. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

9. ISG15 blocks cardiac glycolysis and ensures sufficient mitochondrial energy production during Coxsackievirus B3 infection.

Author

Bredow C, Thery F, Wirth EK, Ochs S, Kespohl M, Kleinau G, Kelm N, Gimber N, Schmoranzer J, Voss M, Klingel K, Spranger J, Renko K, Ralser M, Mülleder M, Heuser A, Knobeloch KP, Scheerer P, Kirwan J, Brüning U, Berndt N, Impens F, and Beling A

Subjects

Animals, Humans, Male, Disease Models, Animal, Enterovirus B, Human pathogenicity, Enterovirus B, Human metabolism, Host-Pathogen Interactions, Mice, Inbred C57BL, Mice, Knockout, Protein Processing, Post-Translational, Signal Transduction, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Coxsackievirus Infections genetics, Cytokines genetics, Cytokines metabolism, Energy Metabolism, Glycolysis, Mitochondria, Heart metabolism, Mitochondria, Heart pathology, Myocytes, Cardiac metabolism, Myocytes, Cardiac virology, Myocytes, Cardiac pathology, Ubiquitins metabolism, Ubiquitins genetics

Abstract

Aims: Virus infection triggers inflammation and, may impose nutrient shortage to the heart. Supported by type I interferon (IFN) signalling, cardiomyocytes counteract infection by various effector processes, with the IFN-stimulated gene of 15 kDa (ISG15) system being intensively regulated and protein modification with ISG15 protecting mice Coxsackievirus B3 (CVB3) infection. The underlying molecular aspects how the ISG15 system affects the functional properties of respective protein substrates in the heart are unknown., Methods and Results: Based on the protective properties due to protein ISGylation, we set out a study investigating CVB3-infected mice in depth and found cardiac atrophy with lower cardiac output in ISG15-/- mice. By mass spectrometry, we identified the protein targets of the ISG15 conjugation machinery in heart tissue and explored how ISGylation affects their function. The cardiac ISGylome showed a strong enrichment of ISGylation substrates within glycolytic metabolic processes. Two control enzymes of the glycolytic pathway, hexokinase 2 (HK2) and phosphofructokinase muscle form (PFK1), were identified as bona fide ISGylation targets during infection. In an integrative approach complemented with enzymatic functional testing and structural modelling, we demonstrate that protein ISGylation obstructs the activity of HK2 and PFK1. Seahorse-based investigation of glycolysis in cardiomyocytes revealed that, by conjugating proteins, the ISG15 system prevents the infection-/IFN-induced up-regulation of glycolysis. We complemented our analysis with proteomics-based advanced computational modelling of cardiac energy metabolism. Our calculations revealed an ISG15-dependent preservation of the metabolic capacity in cardiac tissue during CVB3 infection. Functional profiling of mitochondrial respiration in cardiomyocytes and mouse heart tissue by Seahorse technology showed an enhanced oxidative activity in cells with a competent ISG15 system., Conclusion: Our study demonstrates that ISG15 controls critical nodes in cardiac metabolism. ISG15 reduces the glucose demand, supports higher ATP production capacity in the heart, despite nutrient shortage in infection, and counteracts cardiac atrophy and dysfunction., Competing Interests: Conflict of interest: JK conducts paid consultancy for Centogene GmbH. All other authors declare no conflict of interest. The patent application EP21174633 with the title “Computer assisted method for the evaluation of cardiac metabolism” was filed by Charité – Universitätsmedizin Berlin as the employer of NB and Titus Kuehne, with both holding inventorship for this patent application., (© The Author(s) 2024. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published

2024

10. Major Group-B Enterovirus populations deleted in the noncoding 5' region of genomic RNA modulate activation of the type I interferon pathway in cardiomyocytes and induce myocarditis.

Author

Callon D, Glenet M, Lebreil AL, Heng L, Bouland N, Fichel C, Fornes P, Andreoletti L, and Berri F

Subjects

Animals, Mice, Humans, Immunity, Innate, Signal Transduction, Interferon-beta metabolism, Interferon-beta genetics, Interferon-beta immunology, Male, 5' Untranslated Regions, Myocarditis virology, Myocarditis immunology, Myocarditis genetics, Myocytes, Cardiac virology, Myocytes, Cardiac metabolism, Enterovirus B, Human immunology, Coxsackievirus Infections immunology, Coxsackievirus Infections virology, Coxsackievirus Infections genetics, Interferon Type I metabolism, RNA, Viral genetics, RNA, Viral metabolism

Abstract

Major 5'-terminally deleted (5'TD) RNA forms of group-B coxsackievirus (CVB-5'TD) has been associated with myocarditis in both mice and humans. Although it is known that interferon-β (IFN-β) signaling is critical for an efficient innate immune response against CVB-induced myocarditis, the link between CVB-5'TD RNA forms and type I IFN signaling in cardiomyocytes remains to be explored. In a mouse model of CVB3/28-induced myocarditis, major early-emerging forms of CVB-5'TD RNA have been characterized as replicative viral populations that impair IFN-β production in the heart. Synthetic CVB3/28 RNA forms mimicking each of these major 5'TD virus populations were transfected in mice and have been shown to modulate innate immune responses in the heart and to induce myocarditis in mice. Remarkably, transfection of synthetic viral RNA with deletions in the secondary structures of the 5'-terminal CVB3 RNA domain I, modifying stem-loops "b", "c" or "d", were found to impair IFN-β production in human cardiomyocytes. In addition, the activation of innate immune response by Poly(I:C), was found to restore IFN-β production and to reduce the burden of CVB-5'TD RNA-forms in cardiac tissues, thereby reducing the mortality rate of infected mice. Overall, our results indicate that major early-emerging CVB3 populations deleted in the domain I of genomic RNA, in the 5' noncoding region, modulate the activation of the type I IFN pathway in cardiomyocytes and induce myocarditis in mice. These findings shed new light on the role of replicative CVB-5'TD RNA forms as key pathophysiological factors in CVB-induced human myocarditis., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2024 Callon et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2024

11. Complement components regulates ferroptosis in CVB3 viral myocarditis by interatction with TFRC.

Author

Yi L, Yang Y, Hu Y, Wu Z, Kong M, Zuoyuan B, Xin X, and Yang Z

Subjects

Animals, Mice, Complement C3 genetics, Complement C3 metabolism, Complement C3 pharmacology, Enterovirus B, Human metabolism, Myocardium metabolism, Immunologic Factors pharmacology, Complement C4 metabolism, Complement C4 pharmacology, Receptors, Transferrin, Myocarditis metabolism, Ferroptosis, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Virus Diseases

Abstract

Background: Dysregulated cell death machinery and an excessive inflammatory response in Coxsackievirus B3(CVB3)-infected myocarditis are hallmarks of an abnormal host response. Complement C4 and C3 are considered the central components of the classical activation pathway and often participate in the response process in the early stages of virus infection., Methods: In our study, we constructed a mouse model of CVB3-related viral myocarditis via intraperitoneal injection of Fer-1 and detected myocarditis and ferroptosis markers in the mouse myocardium. Then, we performed co-IP and protein mass spectrometry analyses to explore which components interact with the ferroptosis gene transferrin receptor (TFRC). Finally, functional experiments were conducted to verify the role of complement components in regulating ferroptosis in CVB3 infection., Results: It showed that the ferroptosis inhibitor Fer-1 could alleviate the inflammation in viral myocarditis as well as ferroptosis. Mechanistically, during CVB3 infection, the key factor TFRC was activated and inhibited by Fer-1. Fer-1 effectively prevented the consumption of complement C3 and overload of the complement product C4b. Interestingly, we found that TFRC directly interacts with complement C4, leading to an increase in the product of C4b and a decrease in the downstream complement C3. Functional experiments have also confirmed that regulating the complement C4/C3 pathway can effectively rescue cell ferroptosis caused by CVB3 infection., Conclusions: In this study, we found that ferroptosis occurs through crosstalk with complement C4 in viral myocarditis through interaction with TFRC and that regulating the complement C4/C3 pathway may rescue ferroptosis in CVB3-infected cardiomyocytes., Competing Interests: Declaration of Competing interest The authors declare that they have no conflict of interest., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

12. MicroRNA-22-3p displaces critical host factors from the 5' UTR and inhibits the translation of Coxsackievirus B3 RNA.

Author

Rani P, George B, V S, Biswas S, V M, Pal A, Rajmani RS, and Das S

Subjects

Animals, Humans, Mice, Antiviral Agents metabolism, HeLa Cells, Intestine, Small metabolism, Intestine, Small virology, Viral Tropism genetics, Virus Replication genetics, Cysteine Endopeptidases metabolism, Protocadherins deficiency, Protocadherins genetics, Myocarditis, 5' Untranslated Regions genetics, Coxsackievirus Infections genetics, Coxsackievirus Infections virology, Enterovirus B, Human genetics, Enterovirus B, Human pathogenicity, Enterovirus B, Human physiology, MicroRNAs genetics, MicroRNAs metabolism, RNA, Viral genetics, RNA, Viral metabolism, Protein Biosynthesis, Host Microbial Interactions genetics

Abstract

Coxsackievirus B3 (CVB3) is known to cause acute myocarditis and pancreatitis in humans. We investigated the microRNAs (miRNAs) that can potentially govern the viral life cycle by binding to the untranslated regions (UTRs) of CVB3 RNA. MicroRNA-22-3p was short-listed, as its potential binding site overlapped with the region crucial for recruiting internal ribosome entry site trans -acting factors (ITAFs) and ribosomes. We demonstrate that miR-22-3p binds CVB3 5' UTR, hinders recruitment of key ITAFs on viral mRNA, disrupts the spatial structure required for ribosome recruitment, and ultimately blocks translation. Likewise, cells lacking miR-22-3p exhibited heightened CVB3 infection compared to wild type, confirming its role in controlling infection. Interestingly, miR-22-3p level was found to be increased at 4 hours post-infection, potentially due to the accumulation of viral 2A protease in the early phase of infection. 2A pro enhances the miR-22-3p level to dislodge the ITAFs from the SD-like sequence, rendering the viral RNA accessible for binding of replication factors to switch to replication. Furthermore, one of the cellular targets of miR-22-3p, protocadherin-1 (PCDH1), was significantly downregulated during CVB3 infection. Partial silencing of PCDH1 reduced viral replication, demonstrating its proviral role. Interestingly, upon CVB3 infection in mice, miR-22-3p level was found to be downregulated only in the small intestine, the primary target organ, indicating its possible role in influencing tissue tropism. It appears miR-22-3p plays a dual role during infection by binding viral RNA to aid its life cycle as a viral strategy and by targeting a proviral protein to restrict viral replication as a host response.IMPORTANCECVB3 infection is associated with the development of end-stage heart diseases. Lack of effective anti-viral treatments and vaccines for CVB3 necessitates comprehensive understanding of the molecular players during CVB3 infection. miRNAs have emerged as promising targets for anti-viral strategies. Here, we demonstrate that miR-22-3p binds to 5' UTR and inhibits viral RNA translation at the later stage of infection to promote viral RNA replication. Conversely, as host response, it targets PCDH1, a proviral factor, to discourage viral propagation. miR-22-3p also influences CVB3 tissue tropism. Deciphering the multifaced role of miR-22-3p during CVB3 infection unravels the necessary molecular insights, which can be exploited for novel intervening strategies to curb infection and restrict viral pathogenesis., Competing Interests: The authors declare no conflict of interest.

Published

2024

13. The lncRNA MEG3/miRNA-21/P38MAPK axis inhibits coxsackievirus 3 replication in acute viral myocarditis.

Author

He F, Liu Z, Feng M, Xiao Z, Yi X, Wu J, Liu Z, Wang G, Li L, and Yao H

Subjects

Animals, Humans, Mice, Enterovirus B, Human genetics, Enterovirus B, Human metabolism, HeLa Cells virology, Virus Replication, Coxsackievirus Infections complications, Coxsackievirus Infections genetics, Enterovirus genetics, MicroRNAs genetics, MicroRNAs metabolism, Myocarditis genetics, Myocarditis metabolism, Myocarditis virology, RNA, Long Noncoding genetics, Virus Diseases

Abstract

Evidence is emerging on the roles of long noncoding RNAs (lncRNAs) as regulatory factors in a variety of viral infection processes, but the mechanisms underlying their functions in coxsackievirus group B type3 (CVB3)-induced acute viral myocarditis have not been explicitly delineated. We previously demonstrated that CVB3 infection decreases miRNA-21 expression; however, lncRNAs that regulate the miRNA-21-dependent CVB3 disease process have yet to be identified. To evaluate lncRNAs upstream of miRNA-21, differentially expressed lncRNAs in CVB3-infected mouse hearts were identified by microarray analysis and lncRNA/miRNA-21 interactions were predicted bioinformatically. MEG3 was identified as a candidate miRNA-21-interacting lncRNA upregulated in CVB3-infected mouse hearts. MEG3 expression was verified to be upregulated in HeLa cells 48 h post CVB3 infection and to act as a competitive endogenous RNA of miRNA-21. MEG3 knockdown resulted in the upregulation of miRNA-21, which inhibited CVB3 replication by attenuating P38-MAPK signaling in vitro and in vivo. Knockdown of MEG3 expression before CVB3 infection inhibited viral replication in mouse hearts and alleviated cardiac injury, which improved survival. Furthermore, the knockdown of CREB5, which was predicted bioinformatically to function upstream of MEG3, was demonstrated to decrease MEG3 expression and CVB3 viral replication. This study identifies the function of the lncRNA MEG3/miRNA-21/P38 MAPK axis in the process of CVB3 replication, for which CREB5 could serve as an upstream modulator., Competing Interests: Declaration of Competing Interest All authors declare that they have no competing interests., (Copyright © 2023 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

14. GPR15-mediated T cell recruitment during acute viral myocarditis facilitated virus elimination and improved outcome.

Author

Stoffers B, Wolf H, Bacmeister L, Kupsch S, Vico T, Marchini T, Brehm MA, Yan I, Becher PM, Ardeshirdavani A, Escher F, Kim SV, Klingel K, Kirchhof P, Blankenberg S, Zeller T, Wolf D, Hilgendorf I, Westermann D, and Lindner D

Subjects

Animals, Mice, Inbred C57BL, T-Lymphocytes, Regulatory immunology, Acute Disease, Interferon-gamma metabolism, Mice, T-Lymphocytes, Cytotoxic immunology, T-Lymphocytes, Cytotoxic metabolism, Male, Chemotaxis, Leukocyte genetics, Chemotaxis, Leukocyte immunology, Myocardium metabolism, Myocardium immunology, Myocardium pathology, Signal Transduction, Myocarditis immunology, Myocarditis metabolism, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled metabolism, Receptors, G-Protein-Coupled deficiency, Receptors, G-Protein-Coupled immunology, Mice, Knockout, Coxsackievirus Infections immunology, Coxsackievirus Infections genetics, Disease Models, Animal, Enterovirus B, Human immunology

Abstract

Viral myocarditis is characterized by infiltration of mononuclear cells essential for virus elimination. GPR15 has been identified as a homing receptor for regulatory T cells in inflammatory intestine diseases, but its role in inflammatory heart diseases is still elusive. Here we show that GPR15 deficiency impairs coxsackievirus B3 elimination, leading to adverse cardiac remodeling and dysfunction. Delayed recruitment of regulatory T cells in GPR15-deficient mice was accompanied by prolonged persistence of cytotoxic and regulatory T cells. In addition, RNA sequencing revealed prolonged inflammatory response and altered chemotaxis in knockout mice. In line, we identified GPR15 and its ligand GPR15L as an important chemokine receptor-ligand pair for the recruitment of regulatory and cytotoxic T cells. In summary, the insufficient virus elimination might be caused by a delayed recruitment of T cells as well as delayed interferon-γ expression, resulting in a prolonged inflammatory response and an adverse outcome in GPR15-deficient mice., (© 2023. The Author(s).)

Published

2024

15. Critical roles of parkin and PINK1 in coxsackievirus B3-induced viral myocarditis.

Author

Jin U, Park SJ, Lee BG, Kim JB, Kim SJ, Joe EH, Woo HG, and Park SM

Subjects

Animals, Humans, Mice, Disease Models, Animal, Enterovirus B, Human genetics, Mice, Knockout, Protein Kinases genetics, Ubiquitin-Protein Ligases genetics, Coxsackievirus Infections genetics, Coxsackievirus Infections pathology, Myocarditis genetics, Myocarditis pathology, Virus Diseases

Abstract

Viral myocarditis is an inflammatory disease of the myocardium, often leads to cardiac dysfunction and death. PARKIN (PRKN) and PINK1, well known as Parkinson's disease-associated genes, have been reported to be involved in innate immunity and mitochondrial damage control. Therefore, we investigated the role of parkin and PINK1 in coxsackievirus B3 (CVB3)-induced viral myocarditis because the etiology of myocarditis is related to abnormal immune response to viral infection and mitochondrial damage. After viral infection, the survival was significantly lower and myocardial damage was more severe in parkin knockout (KO) and PINK1 KO mice compared to wild-type (WT) mice. Parkin KO and PINK1 KO showed defective immune cell recruitment and impaired production of antiviral cytokines such as interferon-gamma, allowing increased viral replication. In addition, parkin KO and PINK1 KO mice were more susceptible to CVB3-induced mitochondrial damage than WT mice, resulting in susceptibility to viral-induced cardiac damage. Finally, using publicly available RNA-seq data, we found that pathogenic mutants of the PRKN gene are more common in patients with dilated cardiomyopathy and myocarditis than in controls or the general population. This study will help elucidate the molecular mechanism of CVB3-induced viral myocarditis., Competing Interests: Declaration of competing interest The authors declare no conflict of interest., (Copyright © 2023 Institut Pasteur. Published by Elsevier Masson SAS. All rights reserved.)

Published

2023

16. Macrophage CAPN4 regulates CVB3-induced cardiac inflammation and injury by promoting NLRP3 inflammasome activation and phenotypic transformation to the inflammatory subtype.

Author

Wang Y, Li M, Chen J, Yu Y, Yu Y, Shi H, Liu X, Chen Z, Chen R, and Ge J

Subjects

Animals, Mice, Enterovirus B, Human metabolism, Inflammation genetics, Inflammation metabolism, Macrophages metabolism, NLR Family, Pyrin Domain-Containing 3 Protein genetics, NLR Family, Pyrin Domain-Containing 3 Protein metabolism, NLR Proteins metabolism, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Inflammasomes metabolism, Myocarditis genetics, Myocarditis metabolism

Abstract

Exploring the immune mechanism of coxsackievirus B3 (CVB3)-induced myocarditis may provide a promising therapeutic strategy. Here, we investigated the regulatory role of macrophage CAPN4 in the phenotypic transformation of macrophages and NOD-like receptor protein 3 (NLRP3) inflammasome activation. We found that CAPN4 was the most upregulated subtype of the calpain family in CVB3-infected bone marrow-derived macrophages (BMDMs) and Raw 264.7 cells after CVB3 infection and was upregulated in cardiac macrophages from CVB3-infected mice. Conditional knockout of CAPN4 (CAPN4 flox/flox ; LYZ2-Cre, CAPN4-cKO mice) ameliorated inflammation and myocardial injury and improved cardiac function and survival after CVB3 infection. Enrichment analysis revealed that macrophage differentiation and the interleukin signaling pathway were the most predominant biological processes in macrophages after CVB3 infection. We further found that CVB3 infection and the overexpression of CAPN4 promoted macrophage M1 polarization and NLRP3 inflammasome activation, while CAPN4 knockdown reversed these changes. Correspondingly, CAPN4-cKO alleviated CVB3-induced M1 macrophage transformation and NLRP3 expression and moderately increased M2 transformation in vivo. The culture supernatant of CAPN4-overexpressing or CVB3-infected macrophages impaired cardiac fibroblast function and viability. Moreover, macrophage CAPN4 could upregulate C/EBP-homologous protein (chop) expression, which increased proinflammatory cytokine release by activating the phosphorylation of transducer of activator of transcription 1 (STAT1) and 3 (STAT3). Overall, these results suggest that CAPN4 increases M1-type and inhibits M2-type macrophage polarization through the chop-STAT1/STAT3 signaling pathway to mediate CVB3-induced myocardial inflammation and injury. CAPN4 may be a novel target for viral myocarditis treatment., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

17. Role of RNA Domain Structure and Orientation in the Coxsackievirus B3 Virulence Phenotype.

Author

Phillips L and Tapprich WE

Subjects

Humans, 5' Untranslated Regions, HeLa Cells, Internal Ribosome Entry Sites, Phenotype, Virulence, Virulence Factors, Coxsackievirus Infections genetics, Enterovirus B, Human genetics, RNA, Viral genetics, RNA, Viral metabolism

Abstract

Coxsackievirus B3 (CVB3) is an enterovirus that causes diseases such as pancreatitis and myocarditis in humans. Approximately 10% of the CVB3 RNA genome consists of a highly structured 5' untranslated region (5' UTR) that is organized into six domains and contains a type I internal ribosome entry site (IRES). These features are common to all enteroviruses. Each RNA domain plays a vital role in translation and replication during the viral multiplication cycle. We used SHAPE-MaP chemistry to generate secondary structures of the 5' UTR from the avirulent strain CVB3/GA and the virulent strain CVB3/28. Our comparative models show how key nucleotide substitutions cause major restructuring of domains II and III of the 5' UTR in CVB3/GA. Despite these structural shifts, the molecule maintains several well-characterized RNA elements, which allows persistence of the unique avirulent strain. The results shed light on the 5' UTR regions serving as virulence determinants and those required for fundamental viral mechanisms. We used the SHAPE-MaP data to produce theoretical tertiary models using 3dRNA v2.0. These models suggest a compact conformation of the 5' UTR from the virulent strain CVB3/28 that brings critical domains into close contact. In contrast, the model of the 5' UTR from the avirulent strain CVB3/GA suggests a more extended conformation where the same critical domains are more separated. Our results suggest that the structure and orientation of RNA domains in the 5' UTR are responsible for low-efficiency translation, low viral titers, and absence of virulence observed during infection by CVB3/GA. IMPORTANCE Human enteroviruses, which include five different species and over 100 serotypes, are responsible for diseases ranging from mild respiratory infections to serious infections of pancreas, heart, and neural tissue. All enteroviral RNA genomes have a long and highly structured 5' untranslated region (5' UTR) containing an internal ribosome entry site (IRES). Major virulence determinants are located in the 5' UTR. We present RNA structure models that directly compare the 5' UTR derived from virulent and avirulent strains of the enterovirus coxsackievirus B3 (CVB3). The secondary-structure models show rearrangement of RNA domains known to be virulence determinants and conservation of structure in RNA elements known to be vital for translation and replication in the avirulent strain CVB3/GA. The tertiary-structure models reveal reorientation of RNA domains in CVB3/GA. Identifying the details of structure in these critical RNA domains will help direct antiviral approaches to this major human pathogen., Competing Interests: The authors declare no conflict of interest.

Published

2023

18. Macrophage-Specific Coxsackievirus and Adenovirus Receptor Deletion Enhances Macrophage M1 Polarity in CVB3-Induced Myocarditis.

Author

Shin HH, Jeon ES, and Lim BK

Subjects

Mice, Animals, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha metabolism, Lipopolysaccharides metabolism, Enterovirus B, Human metabolism, Macrophages metabolism, Mice, Knockout, Myocarditis pathology, Coxsackievirus Infections genetics, Coxsackievirus Infections pathology

Abstract

The coxsackievirus and adenovirus receptor (CAR) is very well known as an epithelial tight junction and cardiac intercalated disc protein; it mediates attachment and infection via the coxsackievirus B3 (CVB3) and type 5 adenovirus. Macrophages play important roles in early immunity during viral infections. However, the role of CAR in macrophages is not well studied in relation to CVB3 infection. In this study, the function of CAR was observed in the Raw264.7 mouse macrophage cell line. CAR expression was stimulated by treatment with lipopolysaccharide (LPS) and tumor necrosis factor-α (TNF-α). In thioglycollate-induced peritonitis, the peritoneal macrophage was activated and CAR expression was increased. The macrophage-specific CAR conditional knockout mice (KO) were generated from lysozyme Cre mice. The expression of inflammatory cytokine (IL-1β and TNF-α) was attenuated in the KO mice's peritoneal macrophage after LPS treatment. In addition, the virus was not replicated in CAR-deleted macrophages. The organ virus replication was not significantly different in both wild-type (WT) and KO mice at days three and seven post-infection (p.i). However, the inflammatory M1 polarity genes (IL-1β, IL-6, TNF-α and MCP-1) were significantly increased, with increased rates of myocarditis in the heart of KO mice compared to those of WT mice. In contrast, type1 interferon (IFN-α and β) was significantly decreased in the heart of KO mice. Serum chemokine CXCL-11 was increased in the KO mice at day three p.i. compared to the WT mice. The attenuation of IFN-α and β in macrophage CAR deletion induced higher levels of CXCL-11 and more increased CD4 and CD8 T cells in KO mice hearts compared to those of WT mice at day seven p.i. These results demonstrate that macrophage-specific CAR deletion increased the macrophage M1 polarity and myocarditis in CVB3 infection. In addition, chemokine CXCL-11 expression was increased, and stimulated CD4 and CD8 T cell activity. Macrophage CAR may be important for the regulation of innate-immunity-induced local inflammation in CVB3 infection.

Published

2023

19. LncGBP9 knockdown alleviates myocardial inflammation and apoptosis in mice with acute viral myocarditis via suppressing NF-κB signaling pathway.

Author

Xue Y, Zhang J, Ke J, Zeng L, Cheng K, Han X, Chen F, and Chen F

Subjects

Mice, Animals, NF-kappa B metabolism, Enterovirus B, Human metabolism, Signal Transduction, Inflammation metabolism, Apoptosis, Cytokines metabolism, Mice, Inbred BALB C, Myocarditis genetics, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections pathology

Abstract

Background: Myocardial inflammation and apoptosis are key processes in coxsackievirus B3 (CVB3)-induced acute viral myocarditis (AVMC). Accumulating evidence reveals the essential roles of long noncoding RNAs (lncRNAs) in the pathogenesis of AVMC. Here, we aimed to evaluate the biological functions of a novel lncRNA guanylate-binding protein 9 (lncGBP9) in AVMC progression and further explore its underlying mechanisms., Methods: Initially, mouse models of AVMC were constructed by CVB3 infection. The expression and localization of lncGBP9 in heart tissues were analyzed using RT-qPCR and FISH. Adeno-associated virus serotype 9 (AAV9)-mediated lncGBP9 knockdown was then employed to clarify its roles in survival, cardiac function, and myocardial inflammation and apoptosis. Moreover, the mRNA and protein levels of pro-inflammatory cytokines (TNF-α, IL-6, and IL-1β) were detected by RT-qPCR and ELISA, and the regulation of lncGBP9 knockdown on the NF-κB signaling pathway was investigated by Western blotting. Using an in vitro model of HL-1 cardiomyocytes exposed to CVB3 infection, the effects of lncGBP9 knockdown on cell viability, inflammation, and apoptosis were further evaluated in vitro., Results: Increased lncGBP9 expression was detected in the heart tissues of AVMC mice and CVB3-infected HL-1 cells, and was mainly located in the cytoplasm. Knockdown of lncGBP9 remarkably alleviated the severity of AVMC in CVB3-infected mice, as verified by improved cardiac function, and reduced myocardial inflammation and apoptosis. Additionally, lncGBP9 knockdown suppressed the NF-κB signaling pathway and consequently reduced productions of pro-inflammatory cytokines in vivo. In vitro functional assays further confirmed that lncGBP9 knockdown promoted cell viability, inhibited cell apoptosis, and reduced pro-inflammatory cytokines release in CVB3-infected HL-1 cells through suppressing NF-κB activation., Conclusions: Collectively, lncGBP9 knockdown exerts anti-inflammatory and anti-apoptotic effects in CVB3-induced AVMC, which may be mediated in part via NF-κB signaling pathway. These findings highlight lncGBP9 as an attractive target for therapeutic interventions., (© 2022. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2022

20. Poly(rC) binding protein 1 benefits coxsackievirus B3 infection via suppressing the translation of p62/SQSTM1.

Author

He HY, You Z, Ouyang T, Zhao G, Chen LJ, Wang Q, Li JY, Ye X, Zhang MH, Yang D, Ge XY, and Qiu Y

Subjects

5' Untranslated Regions, Carrier Proteins genetics, DNA-Binding Proteins metabolism, HeLa Cells, Humans, Poly A metabolism, RNA-Binding Proteins metabolism, Sequestosome-1 Protein genetics, Sequestosome-1 Protein metabolism, Virus Replication genetics, Coxsackievirus Infections genetics, Enterovirus B, Human genetics

Abstract

Coxsackievirus B3 (CVB3) is a positive single-strand RNA virus causing myocarditis, pancreatitis and meningitis. During CVB3 infection, various host cellular components, including proteins and non-coding RNAs, interact with the virus and affect viral infection. Poly(rC) binding protein 1 (PCBP1) is a multifunctional RNA binding protein regulating transcription, translation and mRNA stability of a variety of genes. In this study, we observed a significant reduction of PCBP1 protein during CVB3 infection. By bioinformatic prediction and luciferase-assay verification, we confirmed that the expression of PCBP1 was directly inhibited by miR-21, a microRNA upregulated during CVB3 infection. Furthermore, we found that overexpression of PCBP1 promoted CVB3 infection and knocking down of PCBP1 inhibited it. In the subsequent mechanism study, our results revealed that PCBP1 blocked the translation of p62/SQSTM1 (sequestosome 1), an autophagy-receptor protein suppressing CVB3 replication, by interacting with the cis-element in the 5' untranslational region (5' UTR) of p62/SQSTM1. In summary, our studies have identified PCBP1 as a beneficial factor for CVB3 infection. These findings may deepen the understanding of host-virus interactions and provide a potential target for intervention of CVB3 infection., (Copyright © 2022. Published by Elsevier B.V.)

Published

2022

21. TFRC upregulation promotes ferroptosis in CVB3 infection via nucleus recruitment of Sp1.

Author

Yi L, Hu Y, Wu Z, Li Y, Kong M, Kang Z, Zuoyuan B, and Yang Z

Subjects

Antigens, CD genetics, Antigens, CD metabolism, Cell Nucleus metabolism, HeLa Cells, Humans, Receptors, Transferrin genetics, Receptors, Transferrin metabolism, Transcriptional Activation, Up-Regulation, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Enterovirus B, Human, Ferroptosis, Sp1 Transcription Factor genetics, Sp1 Transcription Factor metabolism

Abstract

CVB3 is a single positive-strand enterovirus, and a common pathogen in myocarditis etiology. Although a number of antiviral candidates are under development, specific targeted therapy is not available for CVB3. Ferroptosis is a new type of regulatory cell death discovered in recent years. In this study, our team provided the first evidence that ferroptosis existed in CVB3 infection in vivo and in vitro by iron overload, and massive accumulation of lipid peroxides. Mechanistically, we construct a classical model of HeLa cells following a time-course infection (6, 12, 24, 36, 48 h) with CVB3 (MOI = 10). We demonstrated that the TFRC gene plays an important role in promoting ferroptosis in CVB3 infection and downregulation of TFRC attenuated the ferroptosis. Interestingly, we observed that TFRC was nuclear translocation induced by the CVB3, which was predominantly localized in the cell membrane, but redistributed to the nucleus during CVB3 infection. Moreover, we found that the transcription factor Sp1 was an essential factor that could bind to the TFRC promoter and upregulate the TFRC transcription. Collectively, these results suggest that the Sp1/TFRC/Fe axis may provide a new target for the development of therapies against CVB3 infection., (© 2022. The Author(s).)

Published

2022

22. Ligand-of-Numb protein X1 controls the coxsackievirus B3-induced myocarditis via regulating the stability of coxsackievirus and adenovirus receptor.

Author

Zhang T, Wang C, Wei J, Zhu Z, Wang X, and Sun C

Subjects

Animals, Enterovirus B, Human physiology, Ligands, Membrane Proteins, Mice, Nerve Tissue Proteins, Receptors, Virus, Coxsackievirus Infections genetics, Enterovirus, Myocarditis genetics, Myocarditis metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

Group B coxsackieviruses (CVBs) are the main cause of virus-induced myocarditis. CVBs use coxsackievirus and adenovirus receptor (CAR) for infection and targeting CAR has been shown to ameliorate CVBs-induced myocarditis. Ligand-of-Numb protein X1 (LNX1) is an E3 ubiquitin ligase that was shown to interact with CAR. However, the precise effect of LNX1 on CAR and the roles of LNX1 on CVBs-induced myocarditis remain unknown. In the present study, we generated mice deficient in LNX1 in the heart and evaluated the symptoms of myocarditis after CVB3 infection. We also monitored the expression and ubiquitination of CAR in LNX1-deficient cardiomyocytes after CVBs infection. We found that CVBs infection decreased CAR expression while promoted the expression of LNX1. Mice with deficiency of LNX1 in the heart had normal myocardial development while had deteriorated myocarditis symptoms after CVB3 infection. In LNX1-deficient cardiomyocytes, decreased ubiquitination of CAR and upregulation of CAR were observed after CVB3 infection. In summary, LNX1 controls CVB3-induced myocarditis by regulating the expression of CAR., (© 2022. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2022

23. The Disruption of the Endothelial Barrier Contributes to Acute Lung Injury Induced by Coxsackievirus A2 Infection in Mice.

Author

Ji W, Hu Q, Zhang M, Zhang C, Chen C, Yan Y, Zhang X, Chen S, Tao L, Zhang W, Jin Y, and Duan G

Subjects

Acute Lung Injury complications, Acute Lung Injury pathology, Acute Lung Injury virology, Animals, Apoptosis genetics, Claudin-5 genetics, Coxsackievirus Infections complications, Coxsackievirus Infections pathology, Coxsackievirus Infections virology, Cytokines genetics, Disease Models, Animal, Endothelial Cells pathology, Endothelial Cells virology, Hand, Foot and Mouth Disease complications, Hand, Foot and Mouth Disease pathology, Hand, Foot and Mouth Disease virology, Humans, Mice, Occludin genetics, Pulmonary Edema complications, Pulmonary Edema pathology, Pulmonary Edema virology, Tight Junctions genetics, Tight Junctions pathology, Zonula Occludens-1 Protein genetics, p38 Mitogen-Activated Protein Kinases genetics, Acute Lung Injury genetics, Coxsackievirus Infections genetics, Hand, Foot and Mouth Disease genetics, Pulmonary Edema genetics

Abstract

Sporadic occurrences and outbreaks of hand, foot, and mouth disease (HFMD) caused by Coxsackievirus A2 (CVA2) have frequently reported worldwide recently, which pose a great challenge to public health. Epidemiological studies have suggested that the main cause of death in critical patients is pulmonary edema. However, the pathogenesis of this underlying comorbidity remains unclear. In this study, we utilized the 5-day-old BALB/c mouse model of lethal CVA2 infection to evaluate lung damage. We found that the permeability of lung microvascular was significantly increased after CVA2 infection. We also observed the direct infection and apoptosis of lung endothelial cells as well as the destruction of tight junctions between endothelial cells. CVA2 infection led to the degradation of tight junction proteins (e.g., ZO-1, claudin-5, and occludin). The gene transcription levels of von Willebrand factor (vWF), endothelin (ET), thrombomodulin (THBD), granular membrane protein 140 (GMP140), and intercellular cell adhesion molecule-1 (ICAM-1) related to endothelial dysfunction were all significantly increased. Additionally, CVA2 infection induced the increased expression of inflammatory cytokines (IL-6, IL-1β, and MCP-1) and the activation of p38 mitogen-activated protein kinase (MAPK). In conclusion, the disruption of the endothelial barrier contributes to acute lung injury induced by CVA2 infection; targeting p38-MAPK signaling may provide a therapeutic approach for pulmonary edema in critical infections of HFMD.

Published

2021

24. MicroRNA-30a-5p silencing polarizes macrophages toward M2 phenotype to alleviate cardiac injury following viral myocarditis by targeting SOCS1.

Author

Zhang Y, Cai S, Ding X, Lu C, Wu R, Wu H, Shang Y, and Pang M

Subjects

Animals, Antagomirs genetics, Antagomirs metabolism, Cells, Cultured, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Cytokines genetics, Cytokines metabolism, Disease Models, Animal, Enterovirus B, Human pathogenicity, Inflammation Mediators metabolism, Macrophages virology, Male, Mice, Inbred BALB C, MicroRNAs metabolism, Myocarditis genetics, Myocarditis metabolism, Myocarditis virology, Myocytes, Cardiac pathology, Myocytes, Cardiac virology, Phenotype, Signal Transduction, Suppressor of Cytokine Signaling 1 Protein genetics, Mice, Coxsackievirus Infections therapy, Gene Silencing, Genetic Therapy, Macrophages metabolism, MicroRNAs genetics, Myocarditis therapy, Myocytes, Cardiac metabolism, Suppressor of Cytokine Signaling 1 Protein metabolism

Abstract

Viral myocarditis (VMC) is a life-threatening disease characterized by severe cardiac inflammation generally caused by coxsackievirus B3 (CVB3) infection. Several microRNAs (miRNAs or miRs) are known to play crucial roles in the pathogenesis of VMC. The study aimed to decipher the role of miR-30a-5p in the underlying mechanisms of VMC pathogenesis. We first quantified miR-30a-5p expression in a CVB3-induced mouse VMC model. The physiological characteristics of mouse cardiac tissues were then detected by hematoxylin and eosin (HE) and Picrosirius red staining. We established the correlation between miR-30a-5p and SOCS1, using dual-luciferase gene assay and Pearson's correlation coefficient. The expression of inflammatory factors (IFN-γ, IL-6, IL-10, and IL-13), M1 polarization markers [TNF-α, inducible nitric oxide synthase (iNOS)], M2 polarization markers (Arg-1, IL-10), and myocardial hypertrophy markers [atrial natriuretic peptide (ANP) and brain natriuretic peptide (BNP)] was detected by RT-qPCR and Western blot analysis. miR-30a-5p was found to be highly expressed in VMC mice. Silencing of miR-30a-5p improved the cardiac function index and reduced heart weight-to-body weight ratio, myocardial tissue pathological changes and fibrosis degree, serological indexes, as well as proinflammatory factor levels, while enhancing anti-inflammatory factor levels in VMC mice. Furthermore, silencing of miR-30a-5p inhibited M1 polarization of macrophages while promoting M2 polarization in vivo and in vitro. SOCS1 was a target gene of miR-30a-5p, and the aforementioned cardioprotective effects of miR-30a-5p silencing were reversed upon silencing of SOCS1. Overall, this study shows that silencing of miR-30a-5p may promote M2 polarization of macrophages and improve cardiac injury following VMC via SOCS1 upregulation, constituting a potential therapeutic target for VMC treatment. NEW & NOTEWORTHY We found in this study that microRNA (miR)-30a-5p inhibition might improve cardiac injury following viral myocarditis (VMC) by accelerating M2 polarization of macrophages via SOCS1 upregulation. Furthermore, the anti-inflammatory mechanisms of miR-30a-5p inhibition may contribute to the development of new therapeutic strategies for VMC.

Published

2021

25. Comparison of Monoclonal Gammopathies Linked to Poliovirus or Coxsackievirus vs. Other Infectious Pathogens.

Author

Harb J, Mennesson N, Lepetit C, Fourny M, Louvois M, Bosseboeuf A, Allain-Maillet S, Decaux O, Moreau C, Tallet A, Piver E, Moreau P, Salle V, Bigot-Corbel E, and Hermouet S

Subjects

Adult, Aged, Aged, 80 and over, Humans, Middle Aged, Retrospective Studies, Coxsackievirus Infections genetics, Paraproteinemias complications, Poliovirus genetics

Abstract

Chronic stimulation by infectious pathogens or self-antigen glucosylsphingosine (GlcSph) can lead to monoclonal gammopathy of undetermined significance (MGUS) and multiple myeloma (MM). Novel assays such as the multiplex infectious antigen microarray (MIAA) and GlcSph assays, permit identification of targets for >60% purified monoclonal immunoglobulins (Igs). Searching for additional targets, we selected 28 purified monoclonal Igs whose antigen was not represented on the MIAA and GlcSph assays; their specificity of recognition was then analyzed using microarrays consisting of 3760 B-cell epitopes from 196 pathogens. The peptide sequences PALTAVETG and PALTAAETG of the VP1 coat proteins of human poliovirus 1/3 and coxsackievirus B1/B3, respectively, were specifically recognized by 6/28 monoclonal Igs. Re-analysis of patient cohorts showed that purified monoclonal Igs from 10/155 MGUS/SM (6.5%) and 3/147 MM (2.0%) bound to the PALTAVETG or PALTAAETG epitopes. Altogether, PALTAV/AETG-initiated MGUS are not rare and few seem to evolve toward myeloma.

Published

2021

26. A Crucial Role of ACBD3 Required for Coxsackievirus Infection in Animal Model Developed by AAV-Mediated CRISPR Genome Editing Technique.

Author

Shin HJ, Ku KB, Kim S, Kim HS, Kim YS, Kim BT, Kim SJ, and Kim C

Subjects

Adaptor Proteins, Signal Transducing metabolism, Animals, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Dependovirus metabolism, Disease Models, Animal, Enterovirus B, Human physiology, Gene Editing, Gene Knockout Techniques, Humans, Membrane Proteins metabolism, Mice, Mice, Knockout, Adaptor Proteins, Signal Transducing genetics, Clustered Regularly Interspaced Short Palindromic Repeats, Coxsackievirus Infections genetics, Dependovirus genetics, Membrane Proteins genetics

Abstract

Genetic screens using CRISPR/Cas9 have been exploited to discover host-virus interactions. These screens have identified viral dependencies on host proteins during their life cycle and potential antiviral strategies. The acyl-CoA binding domain containing 3 (ACBD3) was identified as an essential host factor for the Coxsackievirus B3 (CVB3) infection. Other groups have also investigated the role of ACBD3 as a host factor for diverse enteroviruses in cultured cells. However, it has not been tested if ACBD3 is required in the animal model of CVB3 infection. Owing to embryonic lethality, conventional knockout mice were not available for in vivo study. As an alternative approach, we used adeno-associated virus (AAV)-mediated CRISPR genome editing to generate mice that lacked ACBD3 within the pancreas, the major target organ for CVB3. Delivery of sgRNAs using self-complementary (sc) AAV8 efficiently induced a loss-of-function mutation in the pancreas of the Cas9 knock-in mice. Loss of ACBD3 in the pancreas resulted in a 100-fold reduction in the CVB3 titer within the pancreas and a noticeable reduction in viral protein expression. These results indicate a crucial function of ACBD3 in CVB3 infection in vivo. AAV-mediated CRISPR genome editing may be applicable to many in vivo studies on the virus-host interaction and identify a novel target for antiviral therapeutics.

Published

2021

27. Two Natural Recombination gave rise to the Coxsackievirus B3 GV that triggered outbreaks in China in 2006 - 2012.

Author

Wang H, Qian Y, Qian C, Dai C, and Shen H

Subjects

China epidemiology, Enterovirus B, Human classification, Humans, Phylogeny, Recombination, Genetic, Serogroup, Coxsackievirus Infections epidemiology, Coxsackievirus Infections genetics, Disease Outbreaks, Enterovirus B, Human genetics

Abstract

Coxsackievirus B3 serotype GV caused the epidemic of Coxsackievirus B3 infection in China from 2006 to 2012. To study the evolution and recombination of Coxsackievirus B3 serotype GV, we performed recombination and phylogenetic analysis of 499 complete genomes of Enterovirus B available in GenBank, dated April 2019. Results indicated that most of the strains of Coxsackievirus B3 GV in P1 region were derived from a Coxsackievirus B3 GVI parent, and in P2-3 region from EchoV E25 strain, with nucleotide identities of 97.2% and 94.7%, respectively. Other strains of Coxsackievirus B3 GV-C1 in P1-P2 regions were derived from Coxsackievirus B3 GV-C3, whereas those in P3 regions were from CVB5. These naturally occurring recombination events were confirmed by phylogenetic analysis. This study indicates that two naturally occurring recombination gave rise to the coxsackievirus B3 GV that triggered outbreaks in China in 2006 - 2012., (Copyright © 2020 Elsevier Masson SAS. All rights reserved.)

Published

2021

28. Coxsackievirus B3 Infection of Human iPSC Lines and Derived Primary Germ-Layer Cells Regarding Receptor Expression.

Author

Böhnke J, Pinkert S, Schmidt M, Binder H, Bilz NC, Jung M, Reibetanz U, Beling A, Rujescu D, and Claus C

Subjects

CD55 Antigens genetics, CD55 Antigens metabolism, Cell Line, Coxsackie and Adenovirus Receptor-Like Membrane Protein genetics, Coxsackievirus Infections genetics, Ectoderm metabolism, Endoderm metabolism, Enterovirus B, Human metabolism, Enterovirus B, Human pathogenicity, Gene Expression Profiling, Germ Layers cytology, Host Microbial Interactions genetics, Humans, Induced Pluripotent Stem Cells virology, Mesoderm metabolism, Oligonucleotide Array Sequence Analysis, RNA genetics, RNA metabolism, Coxsackie and Adenovirus Receptor-Like Membrane Protein metabolism, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Gene Expression Regulation, Developmental genetics, Germ Layers metabolism, Germ Layers virology, Induced Pluripotent Stem Cells metabolism

Abstract

The association of members of the enterovirus family with pregnancy complications up to miscarriages is under discussion. Here, infection of two different human induced pluripotent stem cell (iPSC) lines and iPSC-derived primary germ-layer cells with coxsackievirus B3 (CVB3) was characterized as an in vitro cell culture model for very early human development. Transcriptomic analysis of iPSC lines infected with recombinant CVB3 expressing enhanced green fluorescent protein (EGFP) revealed a reduction in the expression of pluripotency genes besides an enhancement of genes involved in RNA metabolism. The initial distribution of CVB3-EGFP-positive cells within iPSC colonies correlated with the distribution of its receptor coxsackie- and adenovirus receptor (CAR). Application of anti-CAR blocking antibodies supported the requirement of CAR, but not of the co-receptor decay-accelerating factor (DAF) for infection of iPSC lines. Among iPSC-derived germ-layer cells, mesodermal cells were especially vulnerable to CVB3-EGFP infection. Our data implicate further consideration of members of the enterovirus family in the screening program of human pregnancies. Furthermore, iPSCs with their differentiation capacity into cell populations of relevant viral target organs could offer a reliable screening approach for therapeutic intervention and for assessment of organ-specific enterovirus virulence.

Published

2021

29. MicroRNA-30a Modulates Type I Interferon Responses to Facilitate Coxsackievirus B3 Replication Via Targeting Tripartite Motif Protein 25.

Author

Li J, Xie Y, Li L, Li X, Shen L, Gong J, and Zhang R

Subjects

Animals, Capsid Proteins metabolism, Coxsackievirus Infections enzymology, Coxsackievirus Infections genetics, Coxsackievirus Infections immunology, DEAD Box Protein 58 metabolism, Enterovirus B, Human immunology, Enterovirus B, Human metabolism, HEK293 Cells, HeLa Cells, Host-Pathogen Interactions, Humans, Interferon-beta genetics, Mice, Inbred BALB C, MicroRNAs genetics, Myocarditis enzymology, Myocarditis genetics, Myocarditis immunology, Myocytes, Cardiac enzymology, Myocytes, Cardiac immunology, Myocytes, Cardiac virology, Receptors, Immunologic metabolism, Signal Transduction, Transcription Factors genetics, Tripartite Motif Proteins genetics, Ubiquitin-Protein Ligases genetics, Ubiquitination, Up-Regulation, Mice, Coxsackievirus Infections virology, Enterovirus B, Human growth & development, Interferon-beta metabolism, MicroRNAs metabolism, Myocarditis virology, Transcription Factors metabolism, Tripartite Motif Proteins metabolism, Ubiquitin-Protein Ligases metabolism, Virus Replication

Abstract

Viral myocarditis is caused by a viral infection and characterized by the inflammation of the myocardium. Coxsackievirus B3 (CVB3) infection is one of the most common among the infections caused by this virus. The host's early innate immune response to CVB3 infection particularly depends on the functions of type I interferons (IFNs). In this study, we report that a host microRNA, miR-30a, was upregulated by CVB3 to facilitate its replication. We demonstrated that miR-30a was a potent negative regulator of IFN-I signaling by targeting tripartite motif protein 25 (TRIM25). In addition, we found that TRIM25 overexpression significantly suppressed CVB3 replication, whereas TRIM25 knockdown increased viral titer and VP1 protein expression. MiR-30a inhibits the expression of TRIM25 and TRIM25-mediated retinoic acid-inducible gene (RIG)-I ubiquitination to suppress IFN-β activation and production, thereby resulting in the enhancement of CVB3 replication. These results indicate the proviral role of miR-30a in modulating CVB3 infection for the first time. This not only provides a new strategy followed by CVB3 in order to modulate IFN-I-mediated antiviral immune responses by engaging host miR-30a but also improves our understanding of its pathogenesis., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Li, Xie, Li, Li, Shen, Gong and Zhang.)

Published

2021

30. CARD9 mediates T cell inflammatory response in Coxsackievirus B3-induced acute myocarditis.

Author

Sun C, Zhang X, Yu Y, Li Z, and Xie Y

Subjects

Animals, CARD Signaling Adaptor Proteins deficiency, CARD Signaling Adaptor Proteins genetics, Coxsackievirus Infections genetics, Coxsackievirus Infections immunology, Coxsackievirus Infections virology, Cytokines genetics, Cytokines metabolism, Disease Models, Animal, Host-Pathogen Interactions, Inflammation Mediators metabolism, Mice, Inbred C57BL, Mice, Knockout, Myocarditis genetics, Myocarditis immunology, Myocarditis virology, Myocardium immunology, Myocardium pathology, Signal Transduction, T-Lymphocytes immunology, T-Lymphocytes virology, CARD Signaling Adaptor Proteins metabolism, Coxsackievirus Infections metabolism, Enterovirus B, Human immunology, Myocarditis metabolism, Myocardium metabolism, T-Lymphocytes metabolism

Abstract

Cardiac inflammation in Coxsackievirus B3 (CVB3)-induced myocarditis is a consequence of viral-related cardiac injury and immune response. Caspase-associated recruitment domain 9 (CARD9) is a critical adaptor protein involved in transduction of signals from various innate pattern recognition receptors. In this study, the role of CARD9 in acute viral myocarditis was evaluated. CARD9 -/- and C57BL/6 mice were infected with CVB3. On day 7 postinfection, myocardial tissue and blood samples were collected and examined. After CARD9 knockout, mRNA and protein levels of transforming growth factor-β(TGF-β), interleukin-17A(IL-17A), and CARD domain of B-cell CLL/lymphoma 10(BCL-10) in the myocardium were markedly lower in CARD9 -/- mice than in C57BL/6 mice with CVB3-induced viral myocarditis. This trend was similar for the pathological scores for inflammation and serum levels of cytokines interleukin-6(IL-6), interleukin-10(IL-10), interferon -γ(IFN-γ), TGF-β, and IL-17A. These results suggest that the CARD9-mediated secretion of pro-inflammatory cytokines plays an important role in the immune response to acute viral myocarditis., (Copyright © 2020. Published by Elsevier Inc.)

Published

2020

31. Coxsackievirus B Type 4 Infection in β Cells Downregulates the Chaperone Prefoldin URI to Induce a MODY4-like Diabetes via Pdx1 Silencing.

Author

Bernard H, Teijeiro A, Chaves-Pérez A, Perna C, Satish B, Novials A, Wang JP, and Djouder N

Subjects

Animals, Capsid Proteins metabolism, Coxsackievirus Infections metabolism, Coxsackievirus Infections pathology, Coxsackievirus Infections virology, DNA (Cytosine-5-)-Methyltransferase 1 antagonists & inhibitors, DNA (Cytosine-5-)-Methyltransferase 1 metabolism, Diabetes Mellitus, Type 2 metabolism, Diabetes Mellitus, Type 2 pathology, Diabetes Mellitus, Type 2 virology, Disease Models, Animal, Enterovirus B, Human metabolism, Enterovirus B, Human pathogenicity, Female, Gene Expression Regulation, Glucose metabolism, Glucose pharmacology, Homeodomain Proteins metabolism, Humans, Insulin-Secreting Cells drug effects, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells pathology, Insulin-Secreting Cells transplantation, Male, Mice, Mice, Transgenic, Procainamide pharmacology, Rats, Repressor Proteins metabolism, Signal Transduction, Trans-Activators metabolism, Transplantation, Heterologous, Capsid Proteins genetics, Coxsackievirus Infections genetics, DNA (Cytosine-5-)-Methyltransferase 1 genetics, Diabetes Mellitus, Type 2 genetics, Enterovirus B, Human genetics, Homeodomain Proteins genetics, Repressor Proteins genetics, Trans-Activators genetics

Abstract

Enteroviruses are suspected to contribute to insulin-producing β cell loss and hyperglycemia-induced diabetes. However, mechanisms are not fully defined. Here, we show that coxsackievirus B type 4 (CVB4) infection in human islet-engrafted mice and in rat insulinoma cells displays loss of unconventional prefoldin RPB5 interactor (URI) and PDX1, affecting β cell function and identity. Genetic URI ablation in the mouse pancreas causes PDX1 depletion in β cells. Importantly, diabetic PDX1 heterozygous mice overexpressing URI in β cells are more glucose tolerant. Mechanistically, URI loss triggers estrogen receptor nuclear translocation leading to DNA methyltransferase 1 (DNMT1) expression, which induces Pdx1 promoter hypermethylation and silencing. Consequently, demethylating agent procainamide-mediated DNMT1 inhibition reinstates PDX1 expression and protects against diabetes in pancreatic URI-depleted mice . Finally, the β cells of human diabetes patients show correlations between viral protein 1 and URI, PDX1, and DNMT1 levels. URI and DNMT1 expression and PDX1 silencing provide a causal link between enterovirus infection and diabetes., Competing Interests: The authors declare no competing interests., (© 2020 The Author(s).)

Published

2020

32. Hepatocytes trap and silence coxsackieviruses, protecting against systemic disease in mice.

Author

Kimura T, Flynn CT, and Whitton JL

Subjects

Animals, Coxsackie and Adenovirus Receptor-Like Membrane Protein deficiency, Coxsackievirus Infections genetics, Coxsackievirus Infections immunology, Coxsackievirus Infections pathology, Dendritic Cells immunology, Dendritic Cells metabolism, Disease Models, Animal, Gene Expression, Immunity, Innate, Interferon-alpha metabolism, Liver metabolism, Liver pathology, Liver virology, Mice, Mice, Knockout, Mortality, Viral Load, Viremia, Coxsackievirus Infections virology, Disease Resistance genetics, Disease Resistance immunology, Enterovirus physiology, Hepatocytes metabolism, Hepatocytes virology, Host-Pathogen Interactions genetics, Host-Pathogen Interactions immunology

Abstract

Previous research suggests that hepatocytes catabolize chemical toxins but do not remove microbial agents, which are filtered out by other liver cells (Kupffer cells and endothelial cells). Here we show that, contrary to current understanding, hepatocytes trap and rapidly silence type B coxsackieviruses (CVBs). In genetically wildtype mice, this activity causes hepatocyte damage, which is alleviated in mice carrying a hepatocyte-specific deletion of the coxsackievirus-adenovirus receptor. However, in these mutant mice, there is a dramatic early rise in blood-borne virus, followed by accelerated systemic disease and increased mortality. Thus, wild type hepatocytes act similarly to a sponge for CVBs, protecting against systemic illness at the expense of their own survival. We speculate that hepatocytes may play a similar role in other viral infections as well, thereby explaining why hepatocytes have evolved their remarkable regenerative capacity. Our data also suggest that, in addition to their many other functions, hepatocytes might be considered an integral part of the innate immune system.

Published

2020

33. Coxsackievirus B4 Exposure Results in Variable Pattern Recognition Response in the Kidneys of Female Non-Obese Diabetic Mice Before Establishment of Diabetes.

Author

Walter DL, Benner SE, Oaks RJ, Thuma JR, Malgor R, Schwartz FL, Coschigano KT, and McCall KD

Subjects

Animals, Diabetes Mellitus, Experimental, Disease Models, Animal, Female, Gene Expression Regulation, Genetic Predisposition to Disease, Host Microbial Interactions, Humans, Kidney pathology, Kidney virology, Kidney Diseases, Cystic genetics, Kidney Diseases, Cystic virology, Mice, Mice, Inbred NOD, Mice, Knockout, Signal Transduction, Coxsackievirus Infections genetics, Diabetes Mellitus, Type 1 genetics, Diabetes Mellitus, Type 1 virology, Enterovirus B, Human, Receptors, Pattern Recognition genetics

Abstract

End-stage renal disease (ESRD) is described by four primary diagnoses, diabetes, hypertension, glomerulonephritis, and cystic kidney disease, all of which have viruses implicated as causative agents. Enteroviruses, such as coxsackievirus (CV), are a common genus of viruses that have been implicated in both diabetes and cystic kidney disease; however, little is known about how CVs cause kidney injury and ESRD or predispose individuals with a genetic susceptibility to type 1 diabetes (T1D) to kidney injury. This study evaluated kidney injury resulting from coxsackievirus B4 (CVB4) inoculation of non-obese diabetic (NOD) mice to glean a better understanding of how viral exposure may predispose individuals with a genetic susceptibility to T1D to kidney injury. The objectives were to assess acute and chronic kidney damage in CVB4-inoculated NOD mice without diabetes. Results indicated the presence of CVB4 RNA in the kidney for at least 14 days post-CVB4 inoculation and a coordinated pattern recognition receptor response, but the absence of an immune response or cytotoxicity. CVB4-inoculated NOD mice also had a higher propensity to develop an increase in mesangial area 17 weeks post-CVB4 inoculation. These studies identified initial gene expression changes in the kidney resulting from CVB4 exposure that may predispose to ESRD. Thus, this study provides an initial characterization of kidney injury resulting from CVB4 inoculation of mice that are genetically susceptible to developing T1D that may one day provide better therapeutic options and predictive measures for patients who are at risk for developing kidney disease from T1D.

Published

2020

34. The protection effects of survivin in the cell model of CVB3-induced viral myocarditis.

Author

Wu R, Wu T, Li P, Wang Q, Shi Y, Zhan Y, Zhang S, Xia T, Wang Z, and Lv H

Subjects

Animals, Animals, Newborn, Caspase 3 metabolism, Caspase 9 metabolism, Cells, Cultured, Coxsackievirus Infections genetics, Coxsackievirus Infections pathology, Coxsackievirus Infections virology, Mice, Inbred BALB C, Myocarditis genetics, Myocarditis pathology, Myocarditis virology, Myocytes, Cardiac pathology, Signal Transduction, Survivin genetics, Time Factors, Apoptosis, Coxsackievirus Infections metabolism, Enterovirus B, Human pathogenicity, Myocarditis metabolism, Myocytes, Cardiac metabolism, Survivin metabolism

Abstract

Viral myocarditis (VMC) is a widely studied but poorly understood inflammatory cardiomyopathy which mainly affects children and young adults and results in adverse outcomes. Cardiomyocyte apoptosis was reported important in the progress of coxsackievirus B3 (CVB3)-induced VMC and the blocking of this process may contribute to the therapeutic effect towards VMC. Therefore, this study was designed to explore whether survivin, one of the strongest antiapoptotic proteins, can protect cardiomyocytes from apoptosis in VMC and to discover its related mechanisms. Here, the cultured neonatal mouse cardiomyocytes (NMCs) were exposed to CVB3 to establish the cell model of VMC and the results of Western Blot showed that the protein expression of survivin in CVB3-infected NMCs varied at different post-infection time. Lentivirus was next used to examine the function of survivin in CVB3-infected NMCs. TUNEL assay demonstrated that the overexpression of survivin interrupted CVB3-induced apoptosis. It was next examined whether caspase-3 and -9 were involved in the antiapoptotic pathway initiated by survivin via Western Blot. The results showed a reverse relationship between the protein expression of survivin and that of cleaved caspase-3 and cleaved caspase-9, suggesting that survivin may attenuate apoptosis through restraining the activity of caspase-3 and -9. Moreover, the supernatant fluid of cultured NMCs was extracted to detect the quantitation of released lactate dehydrogenase (LDH) and a sharp decrease was discovered in the survivin-overexpressed group compared to the CVB3-infected group, indicating a protective role of survivin in the cell model of CVB3-induced myocarditis. This study demonstrated that survivin was triggered by CVB3 infection in NMCs and survivin executed its antiapoptotic effects via caspase-3- and caspase-9-dependent signaling pathway.

Published

2020

35. Naturally occurring variants in the transmembrane and cytoplasmic domains of the human Coxsackie- and adenovirus receptor have no impact on virus internalisation.

Author

Herrmann L, Filip A, Lapuente D, Tenbusch M, Niehaus K, Rudolph V, and Farr M

Subjects

Animals, CHO Cells, Coxsackie and Adenovirus Receptor-Like Membrane Protein chemistry, Coxsackie and Adenovirus Receptor-Like Membrane Protein metabolism, Coxsackievirus Infections metabolism, Cricetulus, Host-Pathogen Interactions, Humans, Protein Domains, Coxsackie and Adenovirus Receptor-Like Membrane Protein genetics, Coxsackievirus Infections genetics, Enterovirus physiology, Mutation, Missense, Virus Internalization

Abstract

The Coxsackie- and adenovirus receptor (CAR) mediates homophilic cell-cell contacts and susceptibility to both human pathogenic viruses through its membrane-distal immunoglobulin domain. In the present study, we screened five missense variants of the human CAR gene for their influence on adenovector or Coxsackievirus entry into Chinese hamster ovary cells. The CAR variants facilitated virus internalisation to a similar extent as wild type CAR. This underlines CAR's presumed invariance and essential physiological role in embryogenesis., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

36. The Pyrimidine Analog FNC Potently Inhibits the Replication of Multiple Enteroviruses.

Author

Xu N, Yang J, Zheng B, Zhang Y, Cao Y, Huan C, Wang S, Chang J, and Zhang W

Subjects

Animals, Azides metabolism, China, Coxsackievirus Infections genetics, Deoxycytidine metabolism, Deoxycytidine pharmacology, Enterovirus metabolism, Enterovirus A, Human genetics, Enterovirus B, Human genetics, Enterovirus B, Human metabolism, Enterovirus Infections virology, Mice, Pyrimidines metabolism, Pyrimidines pharmacology, Viral Load drug effects, Azides pharmacology, Deoxycytidine analogs & derivatives, Enterovirus genetics, Virus Replication drug effects

Abstract

Human enteroviruses (EVs), including coxsackieviruses, the numbered enteroviruses, and echoviruses, cause a wide range of diseases, such as hand, foot, and mouth disease (HFMD), encephalitis, myocarditis, acute flaccid myelitis (AFM), pneumonia, and bronchiolitis. Therefore, broad-spectrum anti-EV drugs are urgently needed to treat EV infection. Here, we demonstrate that FNC (2'-deoxy-2'-β-fluoro-4'-azidocytidine), a small nucleoside analog inhibitor that has been demonstrated to be a potent inhibitor of HIV and entered into a clinical phase II trial in China, potently inhibits the viral replication of a multitude of EVs, including enterovirus 71 (EV71), coxsackievirus A16 (CA16), CA6, EVD68, and coxsackievirus B3 (CVB3), at the nanomolar level. The antiviral mechanism of FNC involves mainly positive- and negative-strand RNA synthesis inhibition by targeting and competitively inhibiting the activity of EV71 viral RNA-dependent RNA polymerase (3D pol ), as demonstrated through quantitative real-time reverse transcription-PCR (RT-qPCR), in vitro 3D pol activity, and isothermal titration calorimetry (ITC) experiments. We further demonstrated that FNC treatment every 2 days with 1 mg/kg of body weight in EV71 and CA16 infection neonatal mouse models successfully protected mice from lethal challenge with EV71 and CA16 viruses and reduced the viral load in various tissues. These findings provide important information for the clinical development of FNC as a broad-spectrum inhibitor of human EV pathogens. IMPORTANCE Human enterovirus (EV) pathogens cause various contagious diseases such as hand, foot, and mouth disease, encephalitis, myocarditis, acute flaccid myelitis, pneumonia, and bronchiolitis, which have become serious health threats. However, except for the EV71 vaccine on the market, there are no effective strategies to prevent and treat other EV pathogen infections. Therefore, broad-spectrum anti-EV drugs are urgently needed. In this study, we demonstrated that FNC, a small nucleoside analog inhibitor that has been demonstrated to be a potent inhibitor of HIV and entered into a clinical phase II trial in China, potently inhibits the viral replication of a multitude of EVs at the nanomolar level. Further investigation revealed that FNC inhibits positive- and negative-strand RNA synthesis of EVs by interacting and interfering with the activity of EV71 viral RNA-dependent RNA polymerase (3D pol ). Our findings demonstrate for the first time that FNC is an effective broad-spectrum inhibitor for human EV pathogens., (Copyright © 2020 Xu et al.)

Published

2020

37. Protein modification with ISG15 blocks coxsackievirus pathology by antiviral and metabolic reprogramming.

Author

Kespohl M, Bredow C, Klingel K, Voß M, Paeschke A, Zickler M, Poller W, Kaya Z, Eckstein J, Fechner H, Spranger J, Fähling M, Wirth EK, Radoshevich L, Thery F, Impens F, Berndt N, Knobeloch KP, and Beling A

Subjects

Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Animals, Coxsackievirus Infections genetics, Cytokines genetics, Female, Gluconeogenesis, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Liver pathology, Liver virology, Mice, Mice, Knockout, RNA-Binding Proteins genetics, RNA-Binding Proteins metabolism, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism, Ubiquitins genetics, Ubiquitins metabolism, Coxsackievirus Infections metabolism, Cytokines metabolism, Enterovirus B, Human metabolism, Liver metabolism, Protein Processing, Post-Translational

Abstract

Protein modification with ISG15 (ISGylation) represents a major type I IFN-induced antimicrobial system. Common mechanisms of action and species-specific aspects of ISGylation, however, are still ill defined and controversial. We used a multiphasic coxsackievirus B3 (CV) infection model with a first wave resulting in hepatic injury of the liver, followed by a second wave culminating in cardiac damage. This study shows that ISGylation sets nonhematopoietic cells into a resistant state, being indispensable for CV control, which is accomplished by synergistic activity of ISG15 on antiviral IFIT1/3 proteins. Concurrent with altered energy demands, ISG15 also adapts liver metabolism during infection. Shotgun proteomics, in combination with metabolic network modeling, revealed that ISG15 increases the oxidative capacity and promotes gluconeogenesis in liver cells. Cells lacking the activity of the ISG15-specific protease USP18 exhibit increased resistance to clinically relevant CV strains, therefore suggesting that stabilizing ISGylation by inhibiting USP18 could be exploited for CV-associated human pathologies., (Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution NonCommercial License 4.0 (CC BY-NC).)

Published

2020

38. Housekeeping Gene Expression in the Fetal and Neonatal Murine Thymus Following Coxsackievirus B4 Infection.

Author

Halouani A, Jmii H, Michaux H, Renard C, Martens H, Pirottin D, Mastouri M, Aouni M, Geenen V, and Jaïdane H

Subjects

Animals, Coxsackievirus Infections metabolism, Mice, Proteins genetics, Proteins metabolism, Transcriptome, Coxsackievirus Infections genetics, Genes, Essential, Thymus Gland metabolism

Abstract

The thymus fulfills the role of T-cell production and differentiation. Studying transcription factors and genes involved in T-cell differentiation and maturation during the fetal and neonatal periods is very important. Nevertheless, no studies to date have been interested in evaluating the expressions of housekeeping genes as internal controls to assess the varying expressions of different genes inside this tissue during that period or in the context of viral infection. Thus, we evaluated by real-time quantitative polymerase chain reaction (qPCR) the expression of the most common internal control genes in the thymus of Swiss albino mice during the fetal and neonatal period, and following in utero infection with Coxsackievirus B4. The stability of expression of these reference genes in different samples was investigated using the geNorm application. Results demonstrated that the expression stability varied greatly between genes. Oaz1 was found to have the highest stability in different stages of development, as well as following Coxsackievirus B4 infection. The current study clearly demonstrated that Oaz1 , with very stable expression levels that outperformed other tested housekeeping genes, could be used as a reference gene in the thymus and thymic epithelial cells during development and following Coxsackievirus B4 infection.

Published

2020

39. Inhibition of microRNA-15 protects H9c2 cells against CVB3-induced myocardial injury by targeting NLRX1 to regulate the NLRP3 inflammasome.

Author

Tong R, Jia T, Shi R, and Yan F

Subjects

Animals, Cell Line, Cell Survival genetics, Coxsackievirus Infections genetics, Creatine Kinase, MB Form metabolism, Cytokines metabolism, Inflammation genetics, L-Lactate Dehydrogenase metabolism, Myocarditis enzymology, Myocarditis genetics, Myocarditis virology, Myocytes, Cardiac enzymology, Rats, Up-Regulation, Apoptosis genetics, Coxsackievirus Infections metabolism, Inflammasomes metabolism, Inflammation metabolism, Myocarditis metabolism, Myocytes, Cardiac metabolism, NLR Family, Pyrin Domain-Containing 3 Protein metabolism

Abstract

Background: Viral myocarditis (VMC) is a type of cardiac inflammation that is generally caused by coxsackievirus B3 (CVB3) infection. Several MicroRNAs (miRNAs) are known to play crucial roles in VMC pathogenesis. MiR-15 is reportedly associated with myocardial injury, inflammatory responses and viral infection. Whether miR-15 affects the occurrence and development of VMC remains largely unknown. The roles of miR-15 and their underlying mechanisms in CVB3-stimulated H9c2 cells were assessed in this study., Methods: We infected H9c2 cells with CVB3 to establish a VMC cellular model. We then determined the effects of miR-15 inhibition on three cardiomyocyte injury markers: lactate dehydrogenase (LDH), creatine kinase-MB (CK-MB) and cardiac troponin-I (cTn-I). The impact on CVB3-induced cell apoptosis and pro-inflammatory cytokines was also investigated. The effects of miR-15 inhibition on NLRP3 inflammasome activation were also assessed. The target relationship between miR-15 and NOD-like receptor X1 (NLRX1) was determined using a luciferase reporter assay., Results: MiR-15 expression was significantly upregulated in H9c2 cells after CVB3 infection. Inhibition of miR-15 significantly decreased the CVB3-induced levels of LDH, CK-MB and cTn-I. It also elevated cell viability, reduced CVB3-induced cell apoptosis and decreased the generation of the interleukins IL-1β, IL-6 and IL-18. Furthermore, we determined that miR-15 inhibition suppressed NLRP3 inflammasome activation by downregulating NLRP3 and caspase-1 p20 expression. We found a direct target relationship between miR-15 and NLRX1. Additionally, inhibition of NLRX1 reversed the protective effects of miR-15 inhibition against CVB3-induced myocardial cell injury by regulating the NLRP3 inflammasome., Conclusion: Our results indicate that miR-15 inhibition alleviates CVB3-induced myocardial inflammation and cell injury. This may be partially due to NLRX1-mediated NLRP3 inflammasome inactivation., Competing Interests: Competing interestsThe authors declare that they have no competing interests., (© The Author(s) 2020.)

Published

2020

40. miR‑217 and miR‑543 downregulation mitigates inflammatory response and myocardial injury in children with viral myocarditis by regulating the SIRT1/AMPK/NF‑κB signaling pathway.

Author

Xia K, Zhang Y, and Sun D

Subjects

AMP-Activated Protein Kinases genetics, AMP-Activated Protein Kinases metabolism, Animals, Cell Line, Child, Child, Preschool, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Down-Regulation, Enterovirus B, Human isolation & purification, Female, Humans, Infant, Male, Mice, Inbred BALB C, Myocarditis metabolism, NF-kappa B genetics, NF-kappa B metabolism, Signal Transduction, Sirtuin 1 genetics, Sirtuin 1 metabolism, Up-Regulation, Coxsackievirus Infections complications, MicroRNAs genetics, Myocarditis genetics, Myocarditis virology

Abstract

The aim of the present study was to investigate the expression levels and roles of microRNA (miR)‑217 and miR‑543 in viral myocarditis, and to examine their underlying mechanisms. Coxsackievirus B3 (CVB3) was used to establish in vivo and in vitro models of viral myocarditis. The levels of miR‑217 and miR‑543 were detected using reverse transcription‑quantitative PCR. The association between miR‑217 and miR‑543 and sirtuin‑1 (SIRT1) was predicted and confirmed by TargetScan and dual‑luciferase reporter assay. Cell viability was detected using Cell Counting Kit‑8 assay, and cell apoptosis was measured by analyzing the expression levels of Bcl‑2 and Bax, and by flow cytometry. In addition, the synthesis of various pro‑inflammatory factors was determined by ELISA. In addition, superoxide dismutase (SOD) activity and malondialdehyde (MDA) levels were measured in cardiomyocytes following transfection and CVB infection. miR‑217 and miR‑543 were found to be highly expressed in the peripheral blood of pediatric patients with viral myocarditis, in the peripheral blood and myocardial tissues of viral myocarditis mice and in CVB3‑infected cardiomyocytes. SIRT1 was found to be a target of both miR‑217 and miR‑543, and SIRT1 expression level was downregulated in viral myocarditis. Further analysis indicated that the reduced cell viability, increased cell apoptosis, enhanced synthesis of inflammatory factors, increased MDA content and decreased SOD activity associated with myocarditis were significantly reversed after inhibition of miR‑217 or miR‑543. Importantly, the present results showed that all the effects of miR‑217 and miR‑543 inhibition on cardiomyocytes were significantly suppressed following SIRT1 knockdown. Collectively, the present data indicated that miR‑217 and miR‑543 were significantly upregulated in viral myocarditis, and downregulation of miR‑217 and miR‑543 attenuated CVB3 infection‑induced cardiomyocyte injury by targeting SIRT1. miR‑217 and miR‑543 may be potential therapeutic targets for developing novel viral myocarditis treatments in the future.

Published

2020

41. Coxsackievirus B3 infection induces changes in the expression of numerous piRNAs.

Author

Yao H, Wang X, Song J, Wang Y, Song Q, and Han J

Subjects

Gene Expression Regulation, HEK293 Cells, HeLa Cells, High-Throughput Nucleotide Sequencing methods, Humans, Sequence Analysis, RNA methods, Coxsackievirus Infections genetics, Enterovirus B, Human pathogenicity, RNA, Small Interfering genetics

Abstract

Piwi-interacting RNAs (piRNAs) play pivotal roles in spermatogenesis and are widely distributed among somatic tissues. However, little is known about piRNAs in HeLa cells infected with coxsackievirus B3 (CVB3). In this study, we systematically investigated changes in piRNA expression in HeLa cells infected with CVB3 using high-throughput sequencing technology. piRNA expression profiles in CVB3-infected HeLa cells were examined at 3, 6 and 9 h postinfection (pi). Of the 32,826 piRNAs that were annotated in the NCBI database, 151,571, 89,698 and 76,626 piRNAs were detected in CVB3-infected HeLa cells at 3, 6 and 9 h pi, respectively. Compared with normal cells, 211, 72 and 94 piRNAs were differentially expressed in CVB3-infected HeLa cells at 3, 6 and 9 h pi, respectively. Thirteen piRNAs, including four novel piRNAs, exhibited concurrent changes in CVB3-infected HeLa cells. The changes in the expression of these 13 piRNAs was confirmed in CVB3-infected HeLa cells and 293T cells by stem-loop RT-qPCR at 3, 6 and 9 h pi. The target genes of 13 piRNAs were predicted. The four novel piRNAs were associated with LTR/ERV, LINE/L1 and LTR/ERVK repetitive elements located on different chromosomes. These findings may promote a better understanding of the regulatory mechanism of pathophysiological changes induced by CVB3 infection.

Published

2020

42. MiR-1/133 attenuates cardiomyocyte apoptosis and electrical remodeling in mice with viral myocarditis.

Author

Li W, Liu M, Zhao C, Chen C, Kong Q, Cai Z, and Li D

Subjects

Animals, Apoptosis Regulatory Proteins genetics, Apoptosis Regulatory Proteins metabolism, Calcium Channels, L-Type genetics, Calcium Channels, L-Type metabolism, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Coxsackievirus Infections virology, Disease Models, Animal, Enterovirus B, Human pathogenicity, Gene Expression Regulation, Ion Channels genetics, Male, Membrane Potentials, Mice, Inbred BALB C, MicroRNAs genetics, Myocarditis genetics, Myocarditis metabolism, Myocarditis virology, Myocytes, Cardiac pathology, Myocytes, Cardiac virology, Potassium Channels, Inwardly Rectifying genetics, Potassium Channels, Inwardly Rectifying metabolism, Shal Potassium Channels genetics, Shal Potassium Channels metabolism, Signal Transduction, Apoptosis, Coxsackievirus Infections prevention & control, Ion Channels metabolism, MicroRNAs metabolism, Myocarditis prevention & control, Myocytes, Cardiac metabolism

Abstract

Background: The role of miR-1 and miR-133 in regulating the expression of potassium and calcium ion channels, and mediating cardiomyocyte apoptosis in mice with viral myocarditis (VMC) is investigated herein., Methods: Male Balb/c mice were randomly divided into groups: control group, VMC group, VMC + miR-1/133 mimics group, or VMC + miR-1/133 negative control (NC) group. VMC was induced with coxsackievirus B3 (CVB3). MiR-1/133 mimics ameliorated cardiac dysfunction in VMC mice and was compared to the VMC+NC group., Results: Hematoxylin and eosin staining showed a well-arranged myocardium without inflammatory cell infiltration in the myocardial matrix of the control group. However, in the VMC and VMC+NC groups, the myocardium was disorganized and swollen with necrosis, and the myocardial matrix was infiltrated with inflammatory cells. These changes were alleviated by miR-1/133 mimics. TUNEL staining revealed decreased cardiomyocyte apoptosis in the VMC + miR-1/133 mimics group compared with the VMC group. In addition, miR-1/133 mimics up-regulated the expression of miR-1 and miR-133, the potassium channel genes Kcnd2 and Kcnj2, as well as Bcl-2, and down-regulated the expression of the potassium channel suppressor gene Irx5, L-type calcium channel subunit gene a1c (Cacna1c), Bax, and caspase-9 in the myocardium of VMC mice. MiR-1/133 also up-regulated the protein levels of Kv4.2 and Kir2.1, and down-regulated the expression of CaV1.2 in the myocardium of VMC mice., Conclusions: MiR-1 and miR-133 decreased cardiomyocyte apoptosis by mediating the expression of apoptosis-related genes in the hearts of VMC mice.

Published

2020

43. Expression Profile and Function Analysis of Long Non-coding RNAs in the Infection of Coxsackievirus B3.

Author

Tong L, Qiu Y, Wang H, Qu Y, Zhao Y, Lin L, Wang Y, Xu W, Zhao W, He H, Zhao G, Zhang MH, Yang D, Ge X, and Zhong Z

Subjects

Gene Expression Profiling, Gene Expression Regulation, Gene Regulatory Networks, HeLa Cells, Host-Pathogen Interactions, Humans, RNA, Messenger genetics, Reproducibility of Results, Virus Replication, Coxsackievirus Infections genetics, Coxsackievirus Infections virology, Enterovirus B, Human physiology, RNA, Long Noncoding genetics

Abstract

The roles of lncRNAs in the infection of enteroviruses have been barely demonstrated. In this study, we used coxsackievirus B3 (CVB3), a typical enterovirus, as a model to investigate the expression profiles and functional roles of lncRNAs in enterovirus infection. We profiled lncRNAs and mRNA expression in CVB3-infected HeLa cells by lncRNA-mRNA integrated microarrays. As a result, 700 differentially expressed lncRNAs (431 up-regulated and 269 down-regulated) and 665 differentially expressed mRNAs (299 up-regulated and 366 down-regulated) were identified in CVB3 infection. Then we performed lncRNA-mRNA integrated pathway analysis to identify potential functional impacts of the differentially expressed mRNAs, in which lncRNA-mRNA correlation network was built. According to lncRNA-mRNA correlation, we found that XLOC-001188, an lncRNA down-regulated in CVB3 infection, was negatively correlated with NFAT5 mRNA, an anti-CVB3 gene reported previously. This interaction was supported by qPCR detection following siRNA-mediated knockdown of XLOC-001188, which showed an increase of NFAT5 mRNA and a reduction of CVB3 genomic RNA. In addition, we observed that four most significantly altered lncRNAs, SNHG11, RP11-145F16.2, RP11-1023L17.1 and RP11-1021N1.2 share several common correlated genes critical for CVB3 infection, such as BRE and IRF2BP1. In all, our studies reveal the alteration of lncRNA expression in CVB3 infection and its potential influence on CVB3 replication, providing useful information for future studies of enterovirus infection.

Published

2019

44. The mammalian host protein DAP5 facilitates the initial round of translation of Coxsackievirus B3 RNA.

Author

Dave P, George B, Raheja H, Rani P, Behera P, and Das S

Subjects

Coxsackievirus Infections genetics, Coxsackievirus Infections virology, Enterovirus B, Human metabolism, Eukaryotic Initiation Factor-4G genetics, Gene Expression Regulation, Viral, HeLa Cells, Host-Pathogen Interactions, Humans, Internal Ribosome Entry Sites, Protein Biosynthesis, RNA, Viral metabolism, Ribosomes metabolism, Ribosomes virology, Coxsackievirus Infections metabolism, Enterovirus B, Human genetics, Eukaryotic Initiation Factor-4G metabolism, RNA, Viral genetics

Abstract

During enteroviral infections, the canonical translation factor eukaryotic translation initiation factor 4 γ I (eIF4GI) is cleaved by viral protease 2A. The resulting C-terminal fragment is recruited by the viral internal ribosome entry site (IRES) for efficient translation of the viral RNA. However, the 2A protease is not present in the viral capsid and is synthesized only after the initial round of translation. This presents the conundrum of how the initial round of translation occurs in the absence of the C-terminal eIF4GI fragment. Interestingly, the host protein DAP5 (also known as p97, eIF4GIII, and eIF4G2), an isoform of eIF4GI, closely resembles the eIF4GI C-terminal fragment produced after 2A protease-mediated cleavage. Using the Coxsackievirus B3 (CVB3) IRES as a model system, here we demonstrate that DAP5, but not the full-length eIF4GI, is required for CVB3 IRES activity for translation of input viral RNA. Additionally, we show that DAP5 is specifically required by type I IRES but not by type II or type III IRES, in which cleavage of eIF4GI has not been observed. We observed that both DAP5 and C-terminal eIF4GI interact with CVB3 IRES in the same region, but DAP5 exhibits a lower affinity for CVB3 IRES compared with the C-terminal eIF4GI fragment. It appears that DAP5 is required for the initial round of viral RNA translation by sustaining a basal level of CVB3 IRES activity. This activity leads to expression of 2A protease and consequent robust CVB3 IRES-mediated translation by the C-terminal eIF4GI fragment., (© 2019 Dave et al.)

Published

2019

45. The protective role of microRNA-21 against coxsackievirus B3 infection through targeting the MAP2K3/P38 MAPK signaling pathway.

Author

He F, Xiao Z, Yao H, Li S, Feng M, Wang W, Liu Z, Liu Z, and Wu J

Subjects

3' Untranslated Regions genetics, Animals, Base Sequence, Caspase 3 metabolism, Enterovirus physiology, Enzyme Activation, HeLa Cells, Host-Pathogen Interactions, Humans, Male, Mice, Inbred BALB C, MicroRNAs genetics, Phosphorylation, Virus Replication, Coxsackievirus Infections enzymology, Coxsackievirus Infections genetics, MAP Kinase Kinase 3 metabolism, MAP Kinase Signaling System, MicroRNAs metabolism, p38 Mitogen-Activated Protein Kinases metabolism

Abstract

Background: The P38 mitogen-activated protein kinase (MAPK) pathway plays an essential role in CVB3-induced diseases. We previously demonstrated microRNA-21 has potential inhibitory effect on the MAP2K3 which locates upstream of P38 MAPK and was upregulated in mouse hearts upon CVB3 infection. However, the effect and underlying mechanism of miRNA-21 on CVB3 infection remain unclear., Methods: We detected continuous changes of cellular miRNA-21 and P38 MAPK proteins expression profiling post CVB3 infection in vitro within 12 h. P38 MAPK signaling was inhibited by the specific inhibitor, small interfering RNA and miRNA-21 mimic in vitro, CVB3 replication, cell apoptosis rate and proliferation were detected. Viral load in the mice heart, cardiomyocyte apoptosis rate and histological of the heart were also detected in the mice model of viral myocarditis pretreated with miRNA-21-lentivirus., Results: We observed significant upregulation of miRNA-21 expression followed by suppression of the MAP2K3/P38 MAPK signaling in CVB3-infected Hela cells. The inactivation of the MAP2K3/P38 MAPK signaling by P38 MAPK specific inhibitor, small interfering RNA against MAP2K3, or miRNA-21 overexpression significantly inhibited viral progeny release from CVB3-infected cells. Mechanistically, when compared with control miRNA, miRNA-21 showed no effect on capsid protein VP1 expression and viral load within host cells, while significantly reversing CVB3-induced caspase-3 activation and cell apoptosis rate, further promoting proliferation of infected cells, which indicates the inhibitory effect of miRNA-21 on CVB3 progeny release. In the in vivo study, when compared with control miRNA, miRNA-21 pretreatment remarkably inactivated the MAP2K3/P38 MAPK signaling in mice and protected them against CVB3 infection as evidenced by significantly alleviated cell apoptosis rate, reduced viral titers, necrosis in the heart as well as by remarkably prolonged survival time., Conclusions: miRNA-21 were reverse correlated with P38 MAPK activation post CVB3 infection, miRNA-21 overexpression significantly inhibited viral progeny release and decreased myocytes apoptosis rate in vitro and in vivo, suggesting that miRNA-21 may serve as a potential therapeutic agent against CVB3 infection through targeting the MAP2K3/P38 MAPK signaling.

Published

2019

46. TRAF6: A player in CVB3-induced myocarditis?

Author

Ursu ON, Beyer T, Sauter M, Fragasso A, Bundschuh S, Klingel K, and Munz B

Subjects

Animals, Coxsackievirus Infections genetics, Enterovirus, HeLa Cells, Humans, Mice, Mice, Inbred C57BL, Mice, Knockout, Myocarditis genetics, NF-kappa B genetics, RNA, Small Interfering, TNF Receptor-Associated Factor 6 genetics, Tumor Necrosis Factor-alpha pharmacology, Coxsackievirus Infections metabolism, Myocarditis metabolism, Myocarditis virology, NF-kappa B metabolism, TNF Receptor-Associated Factor 6 metabolism

Abstract

Coxsackievirus B3 (CVB3) is an important inducer of myocarditis, which, in susceptible individuals, can chronify and eventually lead to the development of dilated cardiomyopathy and heart failure. The respective mechanisms are not completely understood. Here, we analyzed expression of the TRAF6 gene, encoding TNF receptor-associated factor 6 (TRAF6), a signal transduction scaffold protein that acts downstream of cytokine receptors, in heart tissue of susceptible and non-susceptible mouse strains. We found that after infection, TRAF6 expression was upregulated in both non-susceptible C57BL/6 wildtype and susceptible A.BY/SnJ and C57BL/6-TLR3 (-/-) mice, however, to different degrees. In infected HeLa cells, we also found moderately elevated TRAF6 levels after infection, in addition, activity of the transcription factor nuclear factor kappa B (NFκB), which can be activated downstream of TRAF6, was strongly enhanced in infected cells. To functionally analyze the role of TRAF6 with regard to infection progression, TRAF6 expression was knocked down in cultured HeLa cells using specific siRNAs. We found that reduction of TRAF6 expression had no effect on NFκB activation in response to infection. Taken together, our data suggest that CVB3 infection enhances TRAF6 levels, however, this induction might not be necessary for infection-induced NFκB activation., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2019

47. microRNA-34a aggravates coxsackievirus B3-induced apoptosis of cardiomyocytes through the SIRT1-p53 pathway.

Author

Jiang D, Li M, Yu Y, Shi H, and Chen R

Subjects

Animals, Biomarkers, Coxsackievirus Infections genetics, Coxsackievirus Infections virology, Gene Expression Regulation, Neoplastic, Humans, RNA Interference, Rats, Sirtuin 1 genetics, Tumor Suppressor Protein p53 genetics, Apoptosis genetics, Enterovirus B, Human physiology, Myocytes, Cardiac metabolism, Myocytes, Cardiac virology, Signal Transduction, Sirtuin 1 metabolism, Tumor Suppressor Protein p53 metabolism

Abstract

Viral myocarditis is inflammation of the myocardium mainly caused by a viral infection, and coxsackievirus B3 (CVB3) infection is one of the most common. It is well known that cardiomyocyte apoptosis is involved in the pathogenesis of viral myocarditis. microRNAs (miRNAs, miRs) are endogenous noncoding oligoribonucleotides involved in various pathological conditions, and miR-34a is one of the miRNAs causing apoptosis. Whether miR-34a participates in cardiomyocyte apoptosis during CVB3 infection and the underlying mechanisms is still unclear. In this in vitro study, we found that miR-34a expression increased in cardiomyocytes after CVB3 infection. Furthermore, we found that CVB3 infection augmented histone deacetylase 1 (HDAC1) and Bax expression while inhibiting sirtuin 1 (SIRT1) and Bcl-2 expression, along with the acetylated p53 (Ac-p53) upregulation in cardiomyocytes. The above-mentioned phenomenon was reversed by a miR-34a inhibitor after CVB3 infection. In addition, the Ac-p53 amount increased in CVB3-infected cardiomyocytes, and SRT1720 and trichostatin A (TSA) pretreatment decreased Ac-p53 levels. After pifithrin-α pretreatment of CVB3-infected cardiomyocytes, the protein expression level of HDAC1 decreased while that of SIRT1 increased. Moreover, miR-34a expression and CVB3-induced apoptosis of cardiomyocytes were attenuated by pretreatment with SRT1720, TSA, or pifithrin-α, accompanied with Bax downregulation and Bcl-2 upregulation. In summary, these data indicate that miR-34a induces cardiomyocyte apoptosis by downregulating SIRT1, and the activation of the SIRT1-p53 pathway contributes to CVB3-induced apoptosis of cardiomyocytes. Thus, miR-34a might serve as a potential therapeutic target because it promotes cardiomyocyte apoptosis through the SIRT1-p53 signaling pathway., (© 2019 Wiley Periodicals, Inc.)

Published

2019

48. Comparative analysis of putative novel microRNA expression profiles induced by enterovirus 71 and coxsackievirus A16 infections in human umbilical vein endothelial cells using high-throughput sequencing.

Author

Song J, Hu Y, Zheng H, Guo L, Huang X, Jiang X, Li W, Li J, Yang Z, Dong S, and Liu L

Subjects

Cells, Cultured, Computational Biology, Coxsackievirus Infections virology, Enterovirus Infections virology, Gene Expression Profiling methods, Gene Ontology, Gene Regulatory Networks genetics, Hand, Foot and Mouth Disease genetics, Hand, Foot and Mouth Disease virology, High-Throughput Nucleotide Sequencing methods, Host-Pathogen Interactions genetics, Human Umbilical Vein Endothelial Cells, Humans, Coxsackievirus Infections genetics, Enterovirus pathogenicity, Enterovirus A, Human pathogenicity, Enterovirus Infections genetics, MicroRNAs genetics

Abstract

Hand, foot and mouth disease (HFMD) is mainly caused by human enterovirus 71 (EV71) and coxsackievirus A16 (CA16), which circulate alternatively or together in epidemic areas. Although the two viruses exhibit genetic homology, their clinical manifestations have some discrepancies. However, the factors underlying these differences remain unclear. Herein, we mainly focused on the alterations and roles of putative novel miRNAs in human umbilical vein endothelial cells (HUVECs) following EV71 and CA16 infections using high-throughput sequencing. The results identified 247 putative novel, differentially expressed miRNAs, of which only 11 miRNAs presented an opposite trend between the EV71- and CA16-infected samples and were used for target prediction. Gene ontology (GO) and pathway enrichment analysis of the predicted targets displayed the top 15 significant biological processes, molecular functions, cell components and pathways. Subsequently, regulatory miRNA-predicted targets and miRNA-GO and miRNA-pathway networks were constructed to further reveal the complex regulatory mechanisms of the miRNAs during infection. Therefore, our data provide useful insights that will help elucidate the different host-pathogen interactions following EV71 and CA16 infections and may offer novel therapeutic targets for these infections., (Copyright © 2019. Published by Elsevier B.V.)

Published

2019

49. Mucin-1 is required for Coxsackie Virus B3-induced inflammation in pancreatitis.

Author

Liu X, Clemens DL, Grunkemeyer JA, Price JD, O'Connell K, Chapman NM, Storz P, Wen H, Cox JL, Reid WL, Hollingsworth MA, and Thayer S

Subjects

Animals, Coxsackievirus Infections genetics, Coxsackievirus Infections metabolism, Disease Models, Animal, Enterovirus B, Human, Inflammation genetics, Inflammation metabolism, Inflammation virology, Mice, Mice, Knockout, Mucin-1 genetics, Pancreatitis genetics, Pancreatitis metabolism, Receptors, CCR2 genetics, Receptors, CCR2 metabolism, Coxsackievirus Infections virology, Mucin-1 metabolism, Pancreatitis virology

Abstract

The Muc-1 oncoprotein is a tumor-associated mucin often overexpressed in pancreatic cancer. We report that knockout of Muc-1 reduced the degree of pancreatic inflammation that resulted from infection with Coxsackievirus B3 (CVB3) in a mouse model. CVB3-infected Muc-1-deficient (Muc-1 KO ) mice had significantly reduced infiltration of macrophages into the murine pancreas. We found that Muc-1 signaling through NF-κB increased expression of ICAM-1, a pro-inflammatory mediator that recruits macrophages. Further investigation revealed that bone marrow derived macrophages (BMDM) from the Muc-1 KO mice exhibited defective migration properties, in part due to low expression of the C-C motif chemokine receptor (CCR2) and the integrin Very Late Antigen 4 (VLA-4). The results presented here provide novel insight into the role of Muc-1 in regulating the inflammatory response and the cellular microenvironment in pancreatitis.

Published

2019

50. Altered exosomal miR-181d and miR-30a related to the pathogenesis of CVB3 induced myocarditis by targeting SOCS3.

Author

Fan KL, Li MF, Cui F, Feng F, Kong L, Zhang FH, Hao H, Yin MX, and Liu Y

Subjects

3' Untranslated Regions, Animals, Case-Control Studies, Disease Models, Animal, Enterovirus B, Human pathogenicity, Gene Expression Regulation, HeLa Cells, Humans, Male, Mice, Myocarditis genetics, Coxsackievirus Infections genetics, Exosomes genetics, MicroRNAs genetics, Myocarditis virology, Suppressor of Cytokine Signaling 3 Protein genetics

Abstract

Objective: MicroRNAs are a group of gene expression regulators and some of which have been confirmed to be associated with acute viral myocarditis (VM). This study aims to find new biomarkers for VM diagnosis and explore the roles of miRNAs during the pathogenesis of VM., Patients and Methods: 23 patients with acute myocarditis and 12 controls were included in this research. The expression of 10 candidate miRNAs in the serum exosome was examined by qRT-PCR. The direct targets were predicted using bioinformatics tools and then confirmed by dual luciferase assay and immunoblotting. Levels IL-6 of cell culture supernatants were determined by enzyme-linked immunosorbent assay. Six weeks old male mice were injected intraperitoneally with Coxsackievirus B3 (CVB3) and then treated by miRNA inhibitors through tail vein injection., Results: Five miRNAs were found to have disturbed expression in the exosome and may have the potential to be used as biomarker for VM diagnosis. Meanwhile, the expression of miR-30a and -181d was also altered in the cells after CVB3 infection. We identified SOCS3 as a direct target of miR-30a and -181d. Furthermore, during CVB3 infection, up-regulated miR-30a and -181d are related to enhanced IL-6 level via modulating SOCS3 expression. miRNA inhibitors injection increased mice survival rate after CVB3 infection., Conclusions: miR-30a and -181d contribute to the over-activated inflammatory response to viral infection of the heart during coxsackievirus infection.

Published

2019