Your search keyword '"Sun, Yingjie"' showing total 14 results

1. Virus infection and sphingolipid metabolism.

Author

Dai J, Feng Y, Liao Y, Tan L, Sun Y, Song C, Qiu X, and Ding C

Subjects

Humans, Antiviral Agents pharmacology, Immunity, Innate, Animals, Host-Pathogen Interactions, Viruses metabolism, Virus Internalization, Sphingolipids metabolism, Virus Replication, Virus Diseases metabolism

Abstract

Cellular sphingolipids have vital roles in human virus replication and spread as they are exploited by viruses for cell entry, membrane fusion, genome replication, assembly, budding, and propagation. Intracellular sphingolipid biosynthesis triggers conformational changes in viral receptors and facilitates endosomal escape. However, our current understanding of how sphingolipids precisely regulate viral replication is limited, and further research is required to comprehensively understand the relationships between viral replication and endogenous sphingolipid species. Emerging evidence now suggests that targeting and manipulating sphingolipid metabolism enzymes in host cells is a promising strategy to effectively combat viral infections. Additionally, serum sphingolipid species and concentrations could function as potential serum biomarkers to help monitor viral infection status in different patients. In this work, we comprehensively review the literature to clarify how viruses exploit host sphingolipid metabolism to accommodate viral replication and disrupt host innate immune responses. We also provide valuable insights on the development and use of antiviral drugs in this area., 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 © 2024 Elsevier B.V. All rights reserved.)

Published

2024

2. The Ca 2+ -dependent phosphatase calcineurin dephosphorylates TBK1 to suppress antiviral innate immunity.

Author

Qu Y, Wang S, Jiang H, Wang Q, Liao Y, Qiu X, Tan L, Song C, Ding C, Sun Y, and Yang Z

Subjects

Animals, Humans, Calcium Signaling, Cell Line, HEK293 Cells, Interferon Type I metabolism, Interferon Type I immunology, Newcastle Disease immunology, Newcastle Disease virology, Newcastle Disease metabolism, Phosphorylation, Calcineurin metabolism, Calcium metabolism, Immunity, Innate, Newcastle disease virus immunology, Protein Serine-Threonine Kinases metabolism, Protein Serine-Threonine Kinases genetics, Virus Replication

Abstract

Tumor necrosis factor receptor-associated factor family member-associated NF-κB activator-binding kinase 1 (TBK1) plays a key role in the induction of the type 1 interferon (IFN-I) response, which is an important component of innate antiviral defense. Viruses target calcium (Ca 2+ ) signaling networks, which participate in the regulation of the viral life cycle, as well as mediate the host antiviral response. Although many studies have focused on the role of Ca 2+ signaling in the regulation of IFN-I, the relationship between Ca 2+ and TBK1 in different infection models requires further elucidation. Here, we examined the effects of the Newcastle disease virus (NDV)-induced increase in intracellular Ca 2+ levels on the suppression of host antiviral responses. We demonstrated that intracellular Ca 2+ increased significantly during NDV infection, leading to impaired IFN-I production and antiviral immunity through the activation of calcineurin (CaN). Depletion of Ca² + was found to lead to a significant increase in virus-induced IFN-I production resulting in the inhibition of viral replication. Mechanistically, the accumulation of Ca 2+ in response to viral infection increases the phosphatase activity of CaN, which in turn dephosphorylates and inactivates TBK1 in a Ca 2+ -dependent manner. Furthermore, the inhibition of CaN on viral replication was counteracted in TBK1 knockout cells. Together, our data demonstrate that NDV hijacks Ca 2+ signaling networks to negatively regulate innate immunity via the CaN-TBK1 signaling axis. Thus, our findings not only identify the mechanism by which viruses exploit Ca 2+ signaling to evade the host antiviral response but also, more importantly, highlight the potential role of Ca 2+ homeostasis in the viral innate immune response.IMPORTANCEViral infections disrupt intracellular Ca 2+ homeostasis, which affects the regulation of various host processes to create conditions that are conducive for their own proliferation, including the host immune response. The mechanism by which viruses trigger TBK1 activation and IFN-I induction through viral pathogen-associated molecular patterns has been well defined. However, the effects of virus-mediated Ca 2+ imbalance on the IFN-I pathway requires further elucidation, especially with respect to TBK1 activation. Herein, we report that NDV infection causes an increase in intracellular free Ca 2+ that leads to activation of the serine/threonine phosphatase CaN, which subsequently dephosphorylates TBK1 and negatively regulates IFN-I production. Furthermore, depletion of Ca 2+ or inhibition of CaN activity exerts antiviral effects by promoting the production of IFN-I and inhibiting viral replication. Thus, our results reveal the potential role of Ca 2+ in the innate immune response to viruses and provide a theoretical reference for the treatment of viral infectious diseases., Competing Interests: The authors declare no conflict of interest.

Published

2024

3. Newcastle Disease Virus Manipulates Mitochondrial MTHFD2-Mediated Nucleotide Metabolism for Virus Replication.

Author

Tang N, Chen P, Zhao C, Liu P, Tan L, Song C, Qiu X, Liao Y, Liu X, Luo T, Sun Y, and Ding C

Subjects

Animals, Nucleotides metabolism, Serine metabolism, Cell Line, A549 Cells, Humans, Mesocricetus, Gene Knockdown Techniques, Protein Transport genetics, Mitochondria enzymology, Up-Regulation physiology, Methylenetetrahydrofolate Dehydrogenase (NADP) genetics, Methylenetetrahydrofolate Dehydrogenase (NADP) metabolism, Newcastle Disease enzymology, Newcastle Disease physiopathology, Newcastle Disease virology, Newcastle disease virus genetics, Newcastle disease virus metabolism, Virus Replication genetics

Abstract

Viruses require host cell metabolic reprogramming to satisfy their replication demands; however, the mechanism by which the Newcastle disease virus (NDV) remodels nucleotide metabolism to support self-replication remains unknown. In this study, we demonstrate that NDV relies on the oxidative pentose phosphate pathway (oxPPP) and the folate-mediated one-carbon metabolic pathway to support replication. In concert with [1,2- 13 C 2 ] glucose metabolic flow, NDV used oxPPP to promote pentose phosphate synthesis and to increase antioxidant NADPH production. Metabolic flux experiments using [2,3,3- 2 H] serine revealed that NDV increased one-carbon (1C) unit synthesis flux through the mitochondrial 1C pathway. Interestingly, methylenetetrahydrofolate dehydrogenase (MTHFD2) was upregulated as a compensatory mechanism for insufficient serine availability. Unexpectedly, direct knockdown of enzymes in the one-carbon metabolic pathway, except for cytosolic MTHFD1, significantly inhibited NDV replication. Specific complementation rescue experiments on small interfering RNA (siRNA)-mediated knockdown further revealed that only a knockdown of MTHFD2 strongly restrained NDV replication and was rescued by formate and extracellular nucleotides. These findings indicated that NDV replication relies on MTHFD2 to maintain nucleotide availability. Notably, nuclear MTHFD2 expression was increased during NDV infection and could represent a pathway by which NDV steals nucleotides from the nucleus. Collectively, these data reveal that NDV replication is regulated by the c-Myc-mediated 1C metabolic pathway and that the mechanism of nucleotide synthesis for viral replication is regulated by MTHFD2. IMPORTANCE Newcastle disease virus (NDV) is a dominant vector for vaccine and gene therapy that accommodates foreign genes well but can only infect mammalian cells that have undergone cancerous transformation. Understanding the remodeling of nucleotide metabolic pathways in host cells by NDV proliferation provides a new perspective for the precise use of NDV as a vector or in antiviral research. In this study, we demonstrated that NDV replication is strictly dependent on pathways involved in redox homeostasis in the nucleotide synthesis pathway, including the oxPPP and the mitochondrial one-carbon pathway. Further investigation revealed the potential involvement of NDV replication-dependent nucleotide availability in promoting MTHFD2 nuclear localization. Our findings highlight the differential dependence of NDV on enzymes for one-carbon metabolism, and the unique mechanism of action of MTHFD2 in viral replication, thereby providing a novel target for antiviral or oncolytic virus therapy.

Published

2023

4. Ubiquitination on Lysine 247 of Newcastle Disease Virus Matrix Protein Enhances Viral Replication and Virulence by Driving Nuclear-Cytoplasmic Trafficking.

Author

Peng T, Qiu X, Tan L, Yu S, Yang B, Dai J, Liu X, Sun Y, Song C, Liu W, Meng C, Liao Y, Yuan W, Ren T, Liu X, and Ding C

Subjects

Animals, Chickens, Cytoplasm metabolism, Lysine, Models, Molecular, Mutation, Newcastle Disease metabolism, Newcastle Disease virology, Newcastle disease virus metabolism, Nuclear Export Signals, Nuclear Localization Signals, Viral Matrix Proteins chemistry, Viral Matrix Proteins genetics, Virulence, Virus Release, Cell Nucleus metabolism, Newcastle disease virus pathogenicity, Newcastle disease virus physiology, Ubiquitination, Viral Matrix Proteins metabolism, Virus Replication

Abstract

The Newcastle disease virus (NDV) matrix (M) protein is the pivotal element for viral assembly, budding, and proliferation. It traffics through the cellular nucleus but performs its primary function in the cytoplasm. To investigate the biological importance of M protein nuclear-cytoplasmic trafficking and the mechanism involved, the regulatory motif nuclear export signal (NES) and nuclear localization signal (NLS) were analyzed. Here, two types of combined NLSs and NESs were identified within the NDV-M protein. The Herts/33-type M protein was found to mediate efficient nuclear export and stable virus-like particle (VLP) release, while the LaSota-type M protein was retained mostly in the nuclei and showed retarded VLP production. Two critical residues, namely, 247 and 263, within the motif were identified and associated with nuclear export efficiency. We identified, for the first time, residue 247 as an important monoubiquitination site, of which its modification regulates the nuclear-cytoplasmic trafficking of NDV-M. Subsequently, mutant LaSota strains were rescued via reverse genetics, which contained either single or double amino acid substitutions that were similar to the M of Herts/33. The rescued LaSota (rLaSota) strains rLaSota-R247K, -S263R, and -double mutation (DM) showed about 2-fold higher hemagglutination (HA) titers and 10-fold higher 50% egg infective dose (EID 50 ) titers than wild-type (wt) rLaSota. Furthermore, the mean death time (MDT) and intracerebral pathogenicity index (ICPI) values of those recombinant viruses were slightly higher than those of wt rLaSota probably due to their higher proliferation rates. Our findings contribute to a better understanding of the molecular mechanism of the replication and pathogenicity of NDV and even those of all other paramyxoviruses. This information is beneficial for the development of vaccines and therapies for paramyxoviruses. IMPORTANCE Newcastle disease virus (NDV) is a pathogen that is lethal to birds and causes heavy losses in the poultry industry worldwide. The World Organization for Animal Health (OIE) ranked Newcastle disease (ND) as the third most significant poultry disease and the eighth most important wildlife disease in the World Livestock Disease Atlas in 2011. The matrix (M) protein of NDV is very important for viral assembly and maturation. It is interesting that M proteins enter the cellular nucleus before performing their primary function in the cytoplasm. We found that NDV-M has a combined nuclear import and export signal. The ubiquitin modification of a lysine residue within this signal is critical for quick, efficient nuclear export and subsequent viral production. Our findings shed new light on viral replication and open up new possibilities for therapeutics against NDV and other paramyxoviruses; furthermore, we demonstrate a novel approach for improving paramyxovirus vaccines.

Published

2022

5. ATM-mediated DNA double-strand break response facilitated oncolytic Newcastle disease virus replication and promoted syncytium formation in tumor cells.

Author

Ren S, Ur Rehman Z, Gao B, Yang Z, Zhou J, Meng C, Song C, Nair V, Sun Y, and Ding C

Subjects

A549 Cells, Acid Anhydride Hydrolases genetics, Acid Anhydride Hydrolases metabolism, Animals, Ataxia Telangiectasia Mutated Proteins genetics, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Chick Embryo, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, HEK293 Cells, Humans, MRE11 Homologue Protein genetics, MRE11 Homologue Protein metabolism, Neoplasm Proteins genetics, Neoplasms genetics, Neoplasms virology, Nuclear Proteins genetics, Nuclear Proteins metabolism, Signal Transduction genetics, Ataxia Telangiectasia Mutated Proteins metabolism, DNA Breaks, Double-Stranded, Giant Cells metabolism, Giant Cells virology, Neoplasm Proteins metabolism, Neoplasms metabolism, Newcastle disease virus physiology, Oncolytic Viruses physiology, Virus Replication

Abstract

Deoxyribonucleic acid (DNA) damage response (DDR) is the fundamental cellular response for maintaining genomic integrity and suppressing tumorigenesis. The activation of ataxia telangiectasia-mutated (ATM) kinase is central to DNA double-strand break (DSB) for maintaining host-genome integrity in mammalian cells. Oncolytic Newcastle disease virus (NDV) can selectively replicate in tumor cells; however, its influence on the genome integrity of tumor cells is not well-elucidated. Here, we found that membrane fusion and NDV infection triggered DSBs in tumor cells. The late replication and membrane fusion of NDV mechanistically activated the ATM-mediated DSB pathway via the ATM-Chk2 axis, as evidenced by the hallmarks of DSBs, i.e., auto-phosphorylated ATM and phosphorylated H2AX and Chk2. Immunofluorescence data showed that multifaceted ATM-controlled phosphorylation markedly induced the formation of pan-nuclear punctum foci in response to NDV infection and F-HN co-expression. Specific drug-inhibitory experiments on ATM kinase activity further suggested that ATM-mediated DSBs facilitated NDV replication and membrane fusion. We confirmed that the Mre11-RAD50-NBS1 (MRN) complex sensed the DSB signal activation triggered by NDV infection and membrane fusion. The pharmacological inhibition of MRN activity also significantly inhibited intracellular and extracellular NDV replication and syncytia formation. Collectively, these data identified for the first time a direct link between the membrane fusion induced by virus infection and DDR pathways, thereby providing new insights into the efficient replication of oncolytic NDV in tumor cells., Competing Interests: All listed authors declare no competing financial interest.

Published

2020

6. Goose MAVS functions in RIG-I-mediated IFN-β signaling activation.

Author

Sun Y, Mao X, Zheng H, Wu W, Rehman ZU, Liao Y, Meng C, Qiu X, Tan L, Song C, Xu L, Yu S, and Ding C

Subjects

Adaptor Proteins, Signal Transducing genetics, Amino Acid Sequence, Animals, Base Sequence, Cell Line, Cloning, Molecular, HEK293 Cells, Humans, Newcastle Disease immunology, Protein Domains immunology, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Sequence Analysis, DNA, Signal Transduction immunology, Adaptor Proteins, Signal Transducing metabolism, Geese immunology, Interferon-beta metabolism, Newcastle disease virus immunology, Receptors, Retinoic Acid metabolism, Virus Replication immunology

Abstract

Mitochondrial antiviral-signaling protein (MAVS) is an essential adaptor protein in retinoic acid-inducible gene I (RIG-I)-mediated antiviral innate immunity in mammals. In this study, the goose MAVS gene (goMAVS) was identified. The 2019 bp-long goMAVS exhibits 96.2% amino acid similarity compared to the predicted goMAVS. Quantitative real-time polymerase chain reactions showed that goMAVS mRNA was widely expressed in different tissues. The overexpression of goMAVS in goose embryo fibroblast cells up-regulated the mRNA levels of goose interferon-stimulated genes. We concluded that MAVS mediates the activation of type I interferon (IFN) pathway in a species-specific manner. We further demonstrated that a CARD-like domain, transmembrane domain and two previously unidentified domains of goMAVS were essential for the activation of type I IFN pathway. GoMAVS inhibited Newcastle disease virus replication by activating type I IFN pathways, especially at the early stages of infection. Finally, the interaction between goMAVS and goose RIG-I was confirmed. The CARD domain of goMAVS plays a vital role in the interaction. Together, we identified goMAVS as a goRIG-I interactive protein and concluded that goMAVS is involved in the activation of type I IFN pathways in goose cells., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

7. Newcastle disease virus induces G 0 /G 1 cell cycle arrest in asynchronously growing cells.

Author

Wang Y, Wang R, Li Y, Sun Y, Song C, Zhan Y, Tan L, Liao Y, Meng C, Qiu X, and Ding C

Subjects

Cell Division genetics, Cell Proliferation, Cyclin D metabolism, DNA Replication, G1 Phase Cell Cycle Checkpoints, HeLa Cells, Host-Pathogen Interactions, Humans, Newcastle disease virus genetics, Signal Transduction, Transcription Factor CHOP metabolism, Cell Cycle, Cell Cycle Checkpoints, Newcastle disease virus physiology, Resting Phase, Cell Cycle, Virus Replication genetics

Abstract

The cell cycle, as a basic cellular process, is conservatively regulated. Consequently, subversion of the host cell replication cycle is a common strategy employed by many viruses to create a cellular environment favorable for viral replication. Newcastle disease virus (NDV) causes disease in poultry and is also an effective oncolytic agent. However, the effects of NDV infection on cell cycle progression are unknown. In this study, we showed that NDV replication in asynchronized cells resulted in the accumulation of infected cells in the G 0 /G 1 phase of the cell cycle, which benefitted the proliferation of NDV. Examination of various cell cycle-regulatory proteins showed that expression of cyclin D1, was significantly reduced following NDV infection. Importantly, the decreased expression of cyclin D1 was reversed by inhibition of CHOP expression, indicating that induction of the PERK-eIF-2a-ATF4-CHOP signaling pathway was involved in the G 0 /G 1 phase cell cycle arrest observed following NDV infection., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

8. Newcastle disease virus induces stable formation of bona fide stress granules to facilitate viral replication through manipulating host protein translation.

Author

Sun Y, Dong L, Yu S, Wang X, Zheng H, Zhang P, Meng C, Zhan Y, Tan L, Song C, Qiu X, Wang G, Liao Y, and Ding C

Subjects

Animals, Carrier Proteins metabolism, Cells, Cultured, Chickens, DNA Helicases, Eukaryotic Initiation Factor-2 metabolism, HeLa Cells, Humans, Newcastle disease virus metabolism, Newcastle disease virus pathogenicity, Poly(A)-Binding Proteins metabolism, Poly-ADP-Ribose Binding Proteins, Protein Biosynthesis, RNA Helicases, RNA Recognition Motif Proteins, RNA-Binding Proteins, Ribosome Subunits metabolism, T-Cell Intracellular Antigen-1, eIF-2 Kinase metabolism, Cytoplasmic Granules metabolism, Host-Pathogen Interactions, Newcastle disease virus physiology, Virus Replication

Abstract

Mammalian cells respond to various environmental stressors to form stress granules (SGs) by arresting cytoplasmic mRNA, protein translation element, and RNA binding proteins. Virus-induced SGs function in different ways, depending on the species of virus; however, the mechanism of SG regulation of virus replication is not well understood. In this study, Newcastle disease virus (NDV) triggered stable formation of bona fide SGs on HeLa cells through activating the protein kinase R (PKR)/eIF2α pathway. NDV-induced SGs contained classic SG markers T-cell internal antigen (TIA)-1, Ras GTPase-activating protein-binding protein (G3BP)-1, eukaryotic initiation factors, and small ribosomal subunit, which could be disassembled in the presence of cycloheximide. Treatment with nocodazole, a microtubule disruption drug, led to the formation of relatively small and circular granules, indicating that NDV infection induces canonical SGs. Furthermore, the role of SGs on NDV replication was investigated by knockdown of TIA-1 and TIA-1-related (TIAR) protein, the 2 critical components involved in SG formation from the HeLa cells, followed by NDV infection. Results showed that depletion of TIA-1 or TIAR inhibited viral protein synthesis, reduced extracellular virus yields, but increased global protein translation. FISH revealed that NDV-induced SGs contained predominantly cellular mRNA rather than viral mRNA. Deletion of TIA-1 or TIAR reduced NP mRNA levels in polysomes. These results demonstrate that NDV triggers stable formation of bona fide SGs, which benefit viral protein translation and virus replication by arresting cellular mRNA.-Sun, Y., Dong, L., Yu, S., Wang, X., Zheng, H., Zhang, P., Meng, C., Zhan, Y., Tan, L., Song, C., Qiu, X., Wang, G., Liao, Y., Ding, C. Newcastle disease virus induces stable formation of bona fide stress granules to facilitate viral replication through manipulating host protein translation., (© FASEB.)

Published

2017

9. Toll-like receptor 3 inhibits Newcastle disease virus replication through activation of pro-inflammatory cytokines and the type-1 interferon pathway.

Author

Cheng J, Sun Y, Zhang X, Zhang F, Zhang S, Yu S, Qiu X, Tan L, Song C, Gao S, Wu Y, and Ding C

Subjects

Animals, Chickens, Cytokines genetics, Humans, Interferon-beta genetics, NF-kappa B genetics, NF-kappa B metabolism, Newcastle Disease genetics, Newcastle Disease virology, Newcastle disease virus genetics, Poultry Diseases genetics, Poultry Diseases virology, Promoter Regions, Genetic, Toll-Like Receptor 3 genetics, Cytokines metabolism, Interferon-beta metabolism, Newcastle Disease metabolism, Newcastle disease virus physiology, Poultry Diseases metabolism, Toll-Like Receptor 3 metabolism, Virus Replication

Abstract

Newcastle disease virus (NDV) is an avian paramyxovirus that can selectively replicate in and destroy human tumor cells. In this report, we demonstrate that NDV infection in HeLa cells leads to the activation of the pattern recognition Toll-like receptor 3 (TLR3). Overexpression of TLR3 enhanced the activity of the IFN-β promoter and the transcription factor NF-kappa B (NF-κB), thereby decreasing viral protein synthesis and the virus titer. In addition, the reduction of endogenous TLR3 by small interfering RNA (siRNA) increased NDV replication. Similar anti-NDV effects were observed in DF-1 chicken fibroblast cells with the exogenous expression of chicken TLR3 (cTLR3). Immunofluorescence staining of HeLa cells indicated that the dsRNA generated during NDV replication colocalized with TLR3 in punctate subcellular structures. Altogether, our results strongly suggest that TLR3 actively participates in the recognition of the innate pro-inflammatory response after NDV infection and leads to the consequent antiviral cytokine/interferon secretion.

Published

2014

10. Activation of the PKR/eIF2α signaling cascade inhibits replication of Newcastle disease virus.

Author

Zhang S, Sun Y, Chen H, Dai Y, Zhan Y, Yu S, Qiu X, Tan L, Song C, and Ding C

Subjects

Animals, Birds, Cell Line, Humans, RNA, Double-Stranded immunology, RNA, Viral immunology, Eukaryotic Initiation Factor-2 metabolism, Newcastle disease virus immunology, Newcastle disease virus physiology, Signal Transduction, Virus Replication, eIF-2 Kinase metabolism

Abstract

Background: Newcastle Disease virus (NDV) causes severe and economically significant disease in almost all birds. However, factors that affect NDV replication in host cells are poorly understood. NDV generates long double-stranded RNA (dsRNA) molecules during transcription of single-stranded genomic RNA. Protein kinase R (PKR) is activated by dsRNA. The aim of this study was to elucidate the role of PKR in NDV infection., Results: NDV infection led to the activation of dsRNA-dependent PKR and phosphorylation of its substrate, translation initiation factor eIF2α, in a dose-dependent manner by either the lentogenic strain LaSota or a velogenic strain Herts/33. PKR activation coincided with the accumulation of dsRNA induced by NDV infection. PKR knockdown remarkably decreased eIF2α phosphorylation as well as IFN-β mRNA levels, leading to the augmentation of extracellular virus titer. Furthermore, siRNA knockdown or phosphorylation of eIF2α or okadaic acid treatment significantly impaired NDV replication, indicating the critical role of the PKR/eIF2α signaling cascade in NDV infection., Conclusion: PKR is activated by dsRNA generated by NDV infection and inhibits NDV replication by eIF2α phosphorylation. This study provides insight into NDV-host interactions for the development of candidate antiviral strategies.

Published

2014

11. Autophagy benefits the replication of Newcastle disease virus in chicken cells and tissues.

Author

Sun Y, Yu S, Ding N, Meng C, Meng S, Zhang S, Zhan Y, Qiu X, Tan L, Chen H, Song C, and Ding C

Subjects

Animals, Cells, Cultured, Chick Embryo, Microscopy, Electron, Transmission, RNA Interference, Autophagy, Newcastle disease virus physiology, Virus Replication

Abstract

Newcastle disease virus (NDV) is an important avian pathogen. We previously reported that NDV triggers autophagy in U251 glioma cells, resulting in enhanced virus replication. In this study, we investigated whether NDV triggers autophagy in chicken cells and tissues to enhance virus replication. We demonstrated that NDV infection induced steady-state autophagy in chicken-derived DF-1 cells and in primary chicken embryo fibroblast (CEF) cells, evident through increased double- or single-membrane vesicles, the accumulation of green fluorescent protein (GFP)-LC3 dots, and the conversion of LC3-I to LC3-II. In addition, we measured autophagic flux by monitoring p62/SQSTM1 degradation, LC3-II turnover, and GFP-LC3 lysosomal delivery and proteolysis, to confirm that NDV infection induced the complete autophagic process. Inhibition of autophagy by pharmacological inhibitors and RNA interference reduced virus replication, indicating an important role for autophagy in NDV infection. Furthermore, we conducted in vivo experiments and observed the conversion of LC3-I to LC3-II in heart, liver, spleen, lung, and kidney of NDV-infected chickens. Regulation of the induction of autophagy with wortmannin, chloroquine, or starvation treatment affects NDV production and pathogenesis in tissues of both lung and intestine; however, treatment with rapamycin, an autophagy inducer of mammalian cells, showed no detectable changes in chicken cells and tissues. Moreover, administration of the autophagy inhibitor wortmannin increased the survival rate of NDV-infected chickens. Our studies provide strong evidence that NDV infection induces autophagy which benefits NDV replication in chicken cells and tissues.

Published

2014

12. Upregulation of DUSP6 impairs infectious bronchitis virus replication by negatively regulating ERK pathway and promoting apoptosis

Author

Wang, Huan, Liu, Dingxiang, Sun, Yingjie, Meng, Chunchun, Tan, Lei, Song, Cuiping, Qiu, Xusheng, Liu, Weiwei, Ding, Chan, and Ying, Liao

Published

2021

13. Newcastle disease virus employs macropinocytosis and Rab5a-dependent intracellular trafficking to infect DF-1 cells

Author

Ying Liao, Chan Ding, Chunchun Meng, Sun Yingjie, Yuan Zhan, Lei Tan, Xusheng Qiu, Yanmei Yuan, Yuqiang Zhang, and Cuiping Song

Subjects

0301 basic medicine, Oncolytic Newcastle Disease Virus, Dynamins, rac1 GTP-Binding Protein, animal structures, Membrane ruffling, macropinocytosis, media_common.quotation_subject, animal diseases, viruses, Endocytic cycle, Newcastle disease virus, Rab5a, Chick Embryo, Endocytosis, Virus Replication, Clathrin, 03 medical and health sciences, Phosphatidylinositol 3-Kinases, Animals, Internalization, Cells, Cultured, Dynamin, media_common, rab5 GTP-Binding Proteins, 030102 biochemistry & molecular biology, biology, Pinocytosis, biochemical phenomena, metabolism, and nutrition, Virus Internalization, Virology, Actins, 030104 developmental biology, Oncology, embryonic structures, biology.protein, Research Paper

Abstract

Oncolytic Newcastle disease virus (NDV) reportedly employs direct fusion of the viral envelope with the plasma membrane and caveolae-dependent endocytosis to enter cells. Here, we show that macropinocytosis and clathrin-mediated endocytosis are involved in NDV entry into a galline embryonic fibroblast cell line. Upon specific inhibition of clathrin assembly, GTPase dynamin, Na+/H+ exchangers, Ras-related C3 botulinum toxin substrate 1, p21 activated kinase 1 or protein kinase C, entry of NDV and its propagation were suppressed. NDV entry into cells triggers Rac1-Pak1 signaling and elicits actin rearrangement and plasma membrane ruffling. Moreover, NDV internalization within macropinosomes and trafficking involve Rab5a-positive vesicles. This is the first report demonstrating that NDV utilizes clathrin-mediated endocytosis and macropinocytosis as alternative endocytic pathways to enter cells. These findings shed new light on the molecular mechanisms underlying NDV entry into cells, and provide potential targets for NDV-mediated therapy in cancer.

Published

2016

14. Newcastle disease virus induces testicular damage and disrupts steroidogenesis in specific pathogen free roosters

Author

Rehman, Zaib Ur, Ren, Shanhui, Yang, Bin, Yang, Xiaofeng, Butt, Salman Latif, Afzal, Alia, Malik, Muhammad Irfan, Sun, Yingjie, Yu, Shengqing, Meng, Chunchun, and Ding, Chan

Subjects

steroidogenesis, Dewey Decimal Classification::600 | Technik::630 | Landwirtschaft, Veterinärmedizin, animal diseases, viruses, genotype, immune response, male genital system, toll like receptor 3, innate immunity, virus replication, 2. Zero hunger, interferon induced helicase C domain containing protein 1, rooster, messenger RNA, poultry, toll like receptor, interferon, 3. Good health, RNA isolation, beta interferon, poultry farming, real time polymerase chain reaction, erythrocyte count, luteinizing hormone, Porcine reproductive and respiratory syndrome virus, germfree chicken, gamma interferon, steroidogenic acute regulatory protein, alpha1 interferon, cytochrome P450, chicken, animal experiment, Newcastle disease virus, testis tissue, interleukin 8, spermatogonium, Article, animal tissue, histology, reverse transcription polymerase chain reaction, male, melanoma, controlled study, nonhuman, Echinococcus granulosus, animal model, lactic acid, lactate dehydrogenase, toll like receptor 7, spermatogenesis, enzyme linked immunosorbent assay, luteinizing hormone receptor, inflammation, testis disease, testosterone, gene expression, cell vacuole, Newcastle disease, upregulation

Abstract

Newcastle disease (ND), which is caused by Newcastle disease virus (NDV), can cause heavy economic losses to the poultry industry worldwide. It is characterised by extensive pathologies of the digestive, respiratory, and nervous systems and can cause severe damage to the reproductive system of egg-laying hens. However, it is unknown whether NDV replicates in the male reproductive system of chickens and induces any pathologies. In this study, we selected a representative strain (i.e. ZJ1) of the most common genotype (i.e. VII) of NDV to investigate whether NDV can induce histological, hormonal, and inflammatory responses in the testes of specific pathogen free (SPF) roosters. NDV infection increased the expression of toll like receptor TLR3, TLR7, MDA5, IFN-α, IFN-β, IFN-γ, IL-8, and CXCLi1 in the testes of NDV-infected roosters at 5 days post-infection (dpi). Severe histological changes, including decrease in the number of Sertoli cells and individualized, shrunken spermatogonia with pyknotic nuclei, were observed at 3 dpi. At 5 dpi, the spermatogenic columns were disorganized, and there were fewer cells, which were replaced by necrotic cells, lipid vacuoles, and proteinaceous homogenous material. A significant decrease in the plasma concentrations of testosterone and luteinizing hormone (LH) and the mRNA expression of their receptors in the testes, steroidogenic acute regulatory protein, cytochrome P450 side-chain cleavage enzyme, and 3β-hydroxysteroid dehydrogenase in the NDV-infected group was observed relative to those in the control group (P < 0.05). Collectively, these results indicate that NDV infection induces a severe inflammatory response and histological changes, which decrease the steroidogenesis. © 2020 The Author(s).