TRIM18 is a critical regulator of viral myocarditis and organ inflammation

Mingli Fang; Ao Zhang; Yong Du; Wenting Lu; Junying Wang; Laurie J. Minze; Timothy C. Cox; Xian Chang Li; Junji Xing; Zhiqiang Zhang

doi:10.1186/s12929-022-00840-z

TRIM18 is a critical regulator of viral myocarditis and organ inflammation

Mingli Fang, Ao Zhang, Yong Du, Wenting Lu, Junying Wang, Laurie J. Minze, Timothy C. Cox, Xian Chang Li, Junji Xing, Zhiqiang Zhang

Research output: Contribution to journal › Article › peer-review

19 Scopus citations

Abstract

Background: Infections by viruses including severe acute respiratory syndrome coronavirus 2 could cause organ inflammations such as myocarditis, pneumonia and encephalitis. Innate immunity to viral nucleic acids mediates antiviral immunity as well as inflammatory organ injury. However, the innate immune mechanisms that control viral induced organ inflammations are unclear. Methods: To understand the role of the E3 ligase TRIM18 in controlling viral myocarditis and organ inflammation, wild-type and Trim18 knockout mice were infected with coxsackievirus B3 for inducing viral myocarditis, influenza A virus PR8 strain and human adenovirus for inducing viral pneumonia, and herpes simplex virus type I for inducing herpes simplex encephalitis. Mice survivals were monitored, and heart, lung and brain were harvested for histology and immunohistochemistry analysis. Real-time PCR, co-immunoprecipitation, immunoblot, enzyme-linked immunosorbent assay, luciferase assay, flow cytometry, over-expression and knockdown techniques were used to understand the molecular mechanisms of TRIM18 in regulating type I interferon (IFN) production after virus infection in this study. Results: We find that knockdown or deletion of TRIM18 in human or mouse macrophages enhances production of type I IFN in response to double strand (ds) RNA and dsDNA or RNA and DNA virus infection. Importantly, deletion of TRIM18 protects mice from viral myocarditis, viral pneumonia, and herpes simplex encephalitis due to enhanced type I IFN production in vivo. Mechanistically, we show that TRIM18 recruits protein phosphatase 1A (PPM1A) to dephosphorylate TANK binding kinase 1 (TBK1), which inactivates TBK1 to block TBK1 from interacting with its upstream adaptors, mitochondrial antiviral signaling (MAVS) and stimulator of interferon genes (STING), thereby dampening antiviral signaling during viral infections. Moreover, TRIM18 stabilizes PPM1A by inducing K63-linked ubiquitination of PPM1A. Conclusions: Our results indicate that TRIM18 serves as a negative regulator of viral myocarditis, lung inflammation and brain damage by downregulating innate immune activation induced by both RNA and DNA viruses. Our data reveal that TRIM18 is a critical regulator of innate immunity in viral induced diseases, thereby identifying a potential therapeutic target for treatment.

Original language	English (US)
Article number	55
Pages (from-to)	55
Journal	Journal of Biomedical Science
Volume	29
Issue number	1
DOIs	https://doi.org/10.1186/s12929-022-00840-z
State	Published - Jul 31 2022

Keywords

DNA virus
Inflammation
Innate immunity
MAVS
Myocarditis
RNA virus
STING
TBK1
Type I IFN
Ubiquitination
Encephalitis, Herpes Simplex
Myocarditis/genetics
RNA
Humans
Protein Phosphatase 2C
Antiviral Agents
Immunity, Innate
Animals
Inflammation/genetics
Mice
Ubiquitin-Protein Ligases/genetics
Virus Diseases

ASJC Scopus subject areas

Biochemistry, medical
Pharmacology (medical)
Molecular Biology
Clinical Biochemistry
Endocrinology, Diabetes and Metabolism
Cell Biology

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10.1186/s12929-022-00840-z

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title = "TRIM18 is a critical regulator of viral myocarditis and organ inflammation",

abstract = "Background: Infections by viruses including severe acute respiratory syndrome coronavirus 2 could cause organ inflammations such as myocarditis, pneumonia and encephalitis. Innate immunity to viral nucleic acids mediates antiviral immunity as well as inflammatory organ injury. However, the innate immune mechanisms that control viral induced organ inflammations are unclear. Methods: To understand the role of the E3 ligase TRIM18 in controlling viral myocarditis and organ inflammation, wild-type and Trim18 knockout mice were infected with coxsackievirus B3 for inducing viral myocarditis, influenza A virus PR8 strain and human adenovirus for inducing viral pneumonia, and herpes simplex virus type I for inducing herpes simplex encephalitis. Mice survivals were monitored, and heart, lung and brain were harvested for histology and immunohistochemistry analysis. Real-time PCR, co-immunoprecipitation, immunoblot, enzyme-linked immunosorbent assay, luciferase assay, flow cytometry, over-expression and knockdown techniques were used to understand the molecular mechanisms of TRIM18 in regulating type I interferon (IFN) production after virus infection in this study. Results: We find that knockdown or deletion of TRIM18 in human or mouse macrophages enhances production of type I IFN in response to double strand (ds) RNA and dsDNA or RNA and DNA virus infection. Importantly, deletion of TRIM18 protects mice from viral myocarditis, viral pneumonia, and herpes simplex encephalitis due to enhanced type I IFN production in vivo. Mechanistically, we show that TRIM18 recruits protein phosphatase 1A (PPM1A) to dephosphorylate TANK binding kinase 1 (TBK1), which inactivates TBK1 to block TBK1 from interacting with its upstream adaptors, mitochondrial antiviral signaling (MAVS) and stimulator of interferon genes (STING), thereby dampening antiviral signaling during viral infections. Moreover, TRIM18 stabilizes PPM1A by inducing K63-linked ubiquitination of PPM1A. Conclusions: Our results indicate that TRIM18 serves as a negative regulator of viral myocarditis, lung inflammation and brain damage by downregulating innate immune activation induced by both RNA and DNA viruses. Our data reveal that TRIM18 is a critical regulator of innate immunity in viral induced diseases, thereby identifying a potential therapeutic target for treatment.",

keywords = "DNA virus, Inflammation, Innate immunity, MAVS, Myocarditis, RNA virus, STING, TBK1, Type I IFN, Ubiquitination, Encephalitis, Herpes Simplex, Myocarditis/genetics, RNA, Humans, Protein Phosphatase 2C, Antiviral Agents, Immunity, Innate, Animals, Inflammation/genetics, Mice, Ubiquitin-Protein Ligases/genetics, Virus Diseases",

author = "Mingli Fang and Ao Zhang and Yong Du and Wenting Lu and Junying Wang and Minze, {Laurie J.} and Cox, {Timothy C.} and Li, {Xian Chang} and Junji Xing and Zhiqiang Zhang",

note = "Funding Information: The work is supported by the following grants from the National Institutes of Health: R01AI155488 (to Z.Z.); R01AI080779 (to X.C.L.); and R01DE027879 (to T.C.C). J.X. is supported by the American Heart Association Career Development Award 20CDA35260116 (Xing). T.C.C is also supported by an Endowment from the Stowers Family Foundation. Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2022",

month = jul,

day = "31",

doi = "10.1186/s12929-022-00840-z",

language = "English (US)",

volume = "29",

pages = "55",

journal = "Journal of Biomedical Science",

issn = "1021-7770",

publisher = "BioMed Central",

number = "1",

}

TY - JOUR

T1 - TRIM18 is a critical regulator of viral myocarditis and organ inflammation

AU - Fang, Mingli

AU - Zhang, Ao

AU - Du, Yong

AU - Lu, Wenting

AU - Wang, Junying

AU - Minze, Laurie J.

AU - Cox, Timothy C.

AU - Li, Xian Chang

AU - Xing, Junji

AU - Zhang, Zhiqiang

N1 - Funding Information: The work is supported by the following grants from the National Institutes of Health: R01AI155488 (to Z.Z.); R01AI080779 (to X.C.L.); and R01DE027879 (to T.C.C). J.X. is supported by the American Heart Association Career Development Award 20CDA35260116 (Xing). T.C.C is also supported by an Endowment from the Stowers Family Foundation. Publisher Copyright: © 2022, The Author(s).

PY - 2022/7/31

Y1 - 2022/7/31

N2 - Background: Infections by viruses including severe acute respiratory syndrome coronavirus 2 could cause organ inflammations such as myocarditis, pneumonia and encephalitis. Innate immunity to viral nucleic acids mediates antiviral immunity as well as inflammatory organ injury. However, the innate immune mechanisms that control viral induced organ inflammations are unclear. Methods: To understand the role of the E3 ligase TRIM18 in controlling viral myocarditis and organ inflammation, wild-type and Trim18 knockout mice were infected with coxsackievirus B3 for inducing viral myocarditis, influenza A virus PR8 strain and human adenovirus for inducing viral pneumonia, and herpes simplex virus type I for inducing herpes simplex encephalitis. Mice survivals were monitored, and heart, lung and brain were harvested for histology and immunohistochemistry analysis. Real-time PCR, co-immunoprecipitation, immunoblot, enzyme-linked immunosorbent assay, luciferase assay, flow cytometry, over-expression and knockdown techniques were used to understand the molecular mechanisms of TRIM18 in regulating type I interferon (IFN) production after virus infection in this study. Results: We find that knockdown or deletion of TRIM18 in human or mouse macrophages enhances production of type I IFN in response to double strand (ds) RNA and dsDNA or RNA and DNA virus infection. Importantly, deletion of TRIM18 protects mice from viral myocarditis, viral pneumonia, and herpes simplex encephalitis due to enhanced type I IFN production in vivo. Mechanistically, we show that TRIM18 recruits protein phosphatase 1A (PPM1A) to dephosphorylate TANK binding kinase 1 (TBK1), which inactivates TBK1 to block TBK1 from interacting with its upstream adaptors, mitochondrial antiviral signaling (MAVS) and stimulator of interferon genes (STING), thereby dampening antiviral signaling during viral infections. Moreover, TRIM18 stabilizes PPM1A by inducing K63-linked ubiquitination of PPM1A. Conclusions: Our results indicate that TRIM18 serves as a negative regulator of viral myocarditis, lung inflammation and brain damage by downregulating innate immune activation induced by both RNA and DNA viruses. Our data reveal that TRIM18 is a critical regulator of innate immunity in viral induced diseases, thereby identifying a potential therapeutic target for treatment.

AB - Background: Infections by viruses including severe acute respiratory syndrome coronavirus 2 could cause organ inflammations such as myocarditis, pneumonia and encephalitis. Innate immunity to viral nucleic acids mediates antiviral immunity as well as inflammatory organ injury. However, the innate immune mechanisms that control viral induced organ inflammations are unclear. Methods: To understand the role of the E3 ligase TRIM18 in controlling viral myocarditis and organ inflammation, wild-type and Trim18 knockout mice were infected with coxsackievirus B3 for inducing viral myocarditis, influenza A virus PR8 strain and human adenovirus for inducing viral pneumonia, and herpes simplex virus type I for inducing herpes simplex encephalitis. Mice survivals were monitored, and heart, lung and brain were harvested for histology and immunohistochemistry analysis. Real-time PCR, co-immunoprecipitation, immunoblot, enzyme-linked immunosorbent assay, luciferase assay, flow cytometry, over-expression and knockdown techniques were used to understand the molecular mechanisms of TRIM18 in regulating type I interferon (IFN) production after virus infection in this study. Results: We find that knockdown or deletion of TRIM18 in human or mouse macrophages enhances production of type I IFN in response to double strand (ds) RNA and dsDNA or RNA and DNA virus infection. Importantly, deletion of TRIM18 protects mice from viral myocarditis, viral pneumonia, and herpes simplex encephalitis due to enhanced type I IFN production in vivo. Mechanistically, we show that TRIM18 recruits protein phosphatase 1A (PPM1A) to dephosphorylate TANK binding kinase 1 (TBK1), which inactivates TBK1 to block TBK1 from interacting with its upstream adaptors, mitochondrial antiviral signaling (MAVS) and stimulator of interferon genes (STING), thereby dampening antiviral signaling during viral infections. Moreover, TRIM18 stabilizes PPM1A by inducing K63-linked ubiquitination of PPM1A. Conclusions: Our results indicate that TRIM18 serves as a negative regulator of viral myocarditis, lung inflammation and brain damage by downregulating innate immune activation induced by both RNA and DNA viruses. Our data reveal that TRIM18 is a critical regulator of innate immunity in viral induced diseases, thereby identifying a potential therapeutic target for treatment.

KW - DNA virus

KW - Inflammation

KW - Innate immunity

KW - MAVS

KW - Myocarditis

KW - RNA virus

KW - STING

KW - TBK1

KW - Type I IFN

KW - Ubiquitination

KW - Encephalitis, Herpes Simplex

KW - Myocarditis/genetics

KW - RNA

KW - Humans

KW - Protein Phosphatase 2C

KW - Antiviral Agents

KW - Immunity, Innate

KW - Animals

KW - Inflammation/genetics

KW - Mice

KW - Ubiquitin-Protein Ligases/genetics

KW - Virus Diseases

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DO - 10.1186/s12929-022-00840-z

M3 - Article

C2 - 35909127

AN - SCOPUS:85135193290

SN - 1021-7770

VL - 29

SP - 55

JO - Journal of Biomedical Science

JF - Journal of Biomedical Science

IS - 1

M1 - 55

ER -

TRIM18 is a critical regulator of viral myocarditis and organ inflammation

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