BIOMAT Database Logo BIOMAT Database Logo

MAVS O-GlcNAcylation Is Essential for Host Antiviral Immunity against Lethal RNA Viruses. 2019

Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
State Key Laboratory of Toxicology and Medical Countermeasures, Beijing Institute of Pharmacology and Toxicology, Beijing 100850, China; State Key Laboratory of Proteomics, National Center of Biomedical Analysis, Beijing 100850, China; Beijing Tropical Medicine Research Institute, Beijing Friendship Hospital, Capital Medical University, Beijing 100050, China.

It is known that lethal viruses profoundly manipulate host metabolism, but how the metabolism alternation affects the immediate host antiviral immunity remains elusive. Here, we report that the O-GlcNAcylation of mitochondrial antiviral-signaling protein (MAVS), a key mediator of interferon signaling, is a critical regulation to activate the host innate immunity against RNA viruses. We show that O-GlcNAcylation depletion in myeloid cells renders the host more susceptible to virus infection both in vitro and in vivo. Mechanistically, we demonstrate that MAVS O-GlcNAcylation is required for virus-induced MAVS K63-linked ubiquitination, thereby facilitating IRF3 activation and IFNβ production. We further demonstrate that D-glucosamine, a commonly used dietary supplement, effectively protects mice against a range of lethal RNA viruses, including human influenza virus. Our study highlights a critical role of O-GlcNAcylation in regulating host antiviral immunity and validates D-glucosamine as a potential therapeutic for virus infections.

UI MeSH Term Description Entries
D007113 Immunity, Innate The capacity of a normal organism to remain unaffected by microorganisms and their toxins. It results from the presence of naturally occurring ANTI-INFECTIVE AGENTS, constitutional factors such as BODY TEMPERATURE and immediate acting immune cells such as NATURAL KILLER CELLS. Immunity, Native,Immunity, Natural,Immunity, Non-Specific,Resistance, Natural,Innate Immune Response,Innate Immunity,Immune Response, Innate,Immune Responses, Innate,Immunity, Non Specific,Innate Immune Responses,Native Immunity,Natural Immunity,Natural Resistance,Non-Specific Immunity
D008297 Male Males
D008810 Mice, Inbred C57BL One of the first INBRED MOUSE STRAINS to be sequenced. This strain is commonly used as genetic background for transgenic mouse models. Refractory to many tumors, this strain is also preferred model for studying role of genetic variations in development of diseases. Mice, C57BL,Mouse, C57BL,Mouse, Inbred C57BL,C57BL Mice,C57BL Mice, Inbred,C57BL Mouse,C57BL Mouse, Inbred,Inbred C57BL Mice,Inbred C57BL Mouse
D008813 Mice, Inbred ICR An inbred strain of mouse that is used as a general purpose research strain, for therapeutic drug testing, and for the genetic analysis of CARCINOGEN-induced COLON CANCER. Mice, Inbred ICRC,Mice, ICR,Mouse, ICR,Mouse, Inbred ICR,Mouse, Inbred ICRC,ICR Mice,ICR Mice, Inbred,ICR Mouse,ICR Mouse, Inbred,ICRC Mice, Inbred,ICRC Mouse, Inbred,Inbred ICR Mice,Inbred ICR Mouse,Inbred ICRC Mice,Inbred ICRC Mouse
D009976 Orthomyxoviridae Infections Virus diseases caused by the ORTHOMYXOVIRIDAE. Orthomyxovirus Infections,Infections, Orthomyxoviridae,Infections, Orthomyxovirus,Swine Influenza,Infection, Orthomyxoviridae,Infection, Orthomyxovirus,Influenza, Swine,Orthomyxoviridae Infection,Orthomyxovirus Infection
D011499 Protein Processing, Post-Translational Any of various enzymatically catalyzed post-translational modifications of PEPTIDES or PROTEINS in the cell of origin. These modifications include carboxylation; HYDROXYLATION; ACETYLATION; PHOSPHORYLATION; METHYLATION; GLYCOSYLATION; ubiquitination; oxidation; proteolysis; and crosslinking and result in changes in molecular weight and electrophoretic motility. Amino Acid Modification, Post-Translational,Post-Translational Modification,Post-Translational Protein Modification,Posttranslational Modification,Protein Modification, Post-Translational,Amino Acid Modification, Posttranslational,Post-Translational Amino Acid Modification,Post-Translational Modifications,Post-Translational Protein Processing,Posttranslational Amino Acid Modification,Posttranslational Modifications,Posttranslational Protein Processing,Protein Processing, Post Translational,Protein Processing, Posttranslational,Amino Acid Modification, Post Translational,Modification, Post-Translational,Modification, Post-Translational Protein,Modification, Posttranslational,Modifications, Post-Translational,Modifications, Post-Translational Protein,Modifications, Posttranslational,Post Translational Amino Acid Modification,Post Translational Modification,Post Translational Modifications,Post Translational Protein Modification,Post Translational Protein Processing,Post-Translational Protein Modifications,Processing, Post-Translational Protein,Processing, Posttranslational Protein,Protein Modification, Post Translational,Protein Modifications, Post-Translational
D002522 Chlorocebus aethiops A species of CERCOPITHECUS containing three subspecies: C. tantalus, C. pygerythrus, and C. sabeus. They are found in the forests and savannah of Africa. The African green monkey is the natural host of SIMIAN IMMUNODEFICIENCY VIRUS and is used in AIDS research. African Green Monkey,Cercopithecus aethiops,Cercopithecus griseoviridis,Cercopithecus griseus,Cercopithecus pygerythrus,Cercopithecus sabeus,Cercopithecus tantalus,Chlorocebus cynosuros,Chlorocebus cynosurus,Chlorocebus pygerythrus,Green Monkey,Grivet Monkey,Lasiopyga weidholzi,Malbrouck,Malbrouck Monkey,Monkey, African Green,Monkey, Green,Monkey, Grivet,Monkey, Vervet,Savanah Monkey,Vervet Monkey,Savannah Monkey,African Green Monkey,Chlorocebus cynosuro,Green Monkey, African,Green Monkeys,Grivet Monkeys,Malbrouck Monkeys,Malbroucks,Monkey, Malbrouck,Monkey, Savanah,Monkey, Savannah,Savannah Monkeys,Vervet Monkeys
D005260 Female Females
D005944 Glucosamine 2-Amino-2-Deoxyglucose,Dona,Dona S,Glucosamine Sulfate,Hespercorbin,Xicil,2 Amino 2 Deoxyglucose,Sulfate, Glucosamine
D006367 HeLa Cells The first continuously cultured human malignant CELL LINE, derived from the cervical carcinoma of Henrietta Lacks. These cells are used for, among other things, VIRUS CULTIVATION and PRECLINICAL DRUG EVALUATION assays. Cell, HeLa,Cells, HeLa,HeLa Cell

Related Publications

Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
Zebrafish mavs Is Essential for Antiviral Innate Immunity.
May 2023, Journal of immunology (Baltimore, Md. : 1950),
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
The Endoplasmic Reticulum ATP13A1 is Essential for MAVS-Mediated Antiviral Innate Immunity.
November 2022, Advanced science (Weinheim, Baden-Wurttemberg, Germany),
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
XAF1 Protects Host against Emerging RNA Viruses by Stabilizing IRF1-Dependent Antiviral Immunity.
September 2022, Journal of virology,
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
MAVS Expression in Alveolar Macrophages Is Essential for Host Resistance against Aspergillus fumigatus.
July 2022, Journal of immunology (Baltimore, Md. : 1950),
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
O-GlcNAcylation Is Essential for Autophagy in Cardiomyocytes.
January 2020, Oxidative medicine and cellular longevity,
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
O-GlcNAcylation is essential for therapeutic mitochondrial transplantation.
November 2023, Communications medicine,
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
MOV10 Provides Antiviral Activity against RNA Viruses by Enhancing RIG-I-MAVS-Independent IFN Induction.
May 2016, Journal of immunology (Baltimore, Md. : 1950),
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
The role of O-GlcNAcylation in immunity against infections.
November 2020, Immunology,
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
O-GlcNAc Transferase Links Glucose Metabolism to MAVS-Mediated Antiviral Innate Immunity.
December 2018, Cell host & microbe,
Nan Song, and Qi Qi, and Ruiyuan Cao, and Bingjie Qin, and Bo Wang, and Yuxia Wang, and Lei Zhao, and Wei Li, and Xianli Du, and Feng Liu, and Yunzheng Yan, and Wen Yi, and Hailu Jiang, and Tao Li, and Tao Zhou, and Hui-Yan Li, and Qing Xia, and Xue-Min Zhang, and Wu Zhong, and Ai-Ling Li, and Xiaotao Duan
MAVS Coordination of Antiviral Innate Immunity.
July 2015, Journal of virology,
Copied contents to your clipboard!