Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication

Zhao, Yuan; Ding, Chan; Zhu, Zhenbang; Wang, Wenqiang; Wen, Wei; Favoreel, Herman; Li, Xiangdong

Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication

Yuan Zhao, Chan Ding, Zhenbang Zhu, Wenqiang Wang, Wei Wen, Herman Favoreel (UGent) and Xiangdong Li

(2024) JOURNAL OF VIROLOGY. 98(10).

Author

Yuan Zhao, Chan Ding, Zhenbang Zhu, Wenqiang Wang, Wei Wen, Herman Favoreel (UGent) and Xiangdong Li

Organization

Department of Translational Physiology, Infectiology and Public Health

Project

Viral control of the epitranscriptome: alphaherpesvirus-induced m6A mRNA demethylation
Targeting IL4 signaling as a novel therapeutic strategy in the treatment of T-cell acute lymphoblastic leukemia
Impact of peripheral virus infection on the central nervous system

Abstract

Pseudorabies virus (PRV) utilizes multiple strategies to inhibit type I interferon (IFN-I) production and signaling to achieve innate immune evasion. Among several other functions, mitochondria serve as a crucial immune hub in the initiation of innate antiviral responses. It is currently unknown whether PRV inhibits innate immune responses by manipulating mitochondria. In this study, we found that PRV infection damages mitochondrial structure and function, as shown by mitochondrial membrane potential depolarization, reduction in mitochondrial numbers, and an imbalance in mitochondrial dynamics. In addition, PRV infection triggered PINK1-Parkin-mediated mitophagy to eliminate the impaired mitochondria, which resulted in a suppression of IFN-I production, thereby promoting viral replication. Furthermore, we found that mitophagy resulted in the degradation of the mitochondrial antiviral signaling protein, which is located on the mitochondrial outer membrane. In conclusion, the data of the current study indicate that PRV-induced mitophagy represents a previously uncharacterized PRV evasion mechanism of the IFN-I response, thereby promoting virus replication.IMPORTANCEPseudorabies virus (PRV), a pathogen that induces different disease symptoms and is often fatal in domestic animals and wildlife, has caused great economic losses to the swine industry. Since 2011, different PRV variant strains have emerged in Asia, against which current commercial vaccines may not always provide optimal protection in pigs. In addition, there are indications that some of these PRV variant strains may sporadically infect people. In the current study, we found that PRV infection causes mitochondria injury. This is associated with the induction of mitophagy to eliminate the damaged mitochondria, which results in suppressed antiviral interferon production and signaling. Hence, our study reveals a novel mechanism that is used by PRV to antagonize the antiviral host immune response, providing a theoretical basis that may contribute to the research toward and development of new vaccines and antiviral drugs. Pseudorabies virus (PRV), a pathogen that induces different disease symptoms and is often fatal in domestic animals and wildlife, has caused great economic losses to the swine industry. Since 2011, different PRV variant strains have emerged in Asia, against which current commercial vaccines may not always provide optimal protection in pigs. In addition, there are indications that some of these PRV variant strains may sporadically infect people. In the current study, we found that PRV infection causes mitochondria injury. This is associated with the induction of mitophagy to eliminate the damaged mitochondria, which results in suppressed antiviral interferon production and signaling. Hence, our study reveals a novel mechanism that is used by PRV to antagonize the antiviral host immune response, providing a theoretical basis that may contribute to the research toward and development of new vaccines and antiviral drugs.

Keywords

pseudorabies virus (PRV), mitochondria, mitophagy, MAVS, interferons production inhibition, MITOCHONDRIAL DYNAMICS, PROTEIN

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Citation

Please use this url to cite or link to this publication: http://hdl.handle.net/1854/LU-01JJKNGM63JEKCCPHXMADE8VQF

MLA: Zhao, Yuan, et al. “Pseudorabies Virus Infection Triggers Mitophagy to Dampen the Interferon Response and Promote Viral Replication.” JOURNAL OF VIROLOGY, edited by Anna Ruth Cliffe, vol. 98, no. 10, 2024, doi:10.1128/jvi.01048-24.
APA: Zhao, Y., Ding, C., Zhu, Z., Wang, W., Wen, W., Favoreel, H., & Li, X. (2024). Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication. JOURNAL OF VIROLOGY, 98(10). https://doi.org/10.1128/jvi.01048-24
Chicago author-date: Zhao, Yuan, Chan Ding, Zhenbang Zhu, Wenqiang Wang, Wei Wen, Herman Favoreel, and Xiangdong Li. 2024. “Pseudorabies Virus Infection Triggers Mitophagy to Dampen the Interferon Response and Promote Viral Replication.” Edited by Anna Ruth Cliffe. JOURNAL OF VIROLOGY 98 (10). https://doi.org/10.1128/jvi.01048-24.
Chicago author-date (all authors): Zhao, Yuan, Chan Ding, Zhenbang Zhu, Wenqiang Wang, Wei Wen, Herman Favoreel, and Xiangdong Li. 2024. “Pseudorabies Virus Infection Triggers Mitophagy to Dampen the Interferon Response and Promote Viral Replication.” Ed by. Anna Ruth Cliffe. JOURNAL OF VIROLOGY 98 (10). doi:10.1128/jvi.01048-24.
Vancouver: 1.
Zhao Y, Ding C, Zhu Z, Wang W, Wen W, Favoreel H, et al. Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication. Cliffe AR, editor. JOURNAL OF VIROLOGY. 2024;98(10).
IEEE: [1]
Y. Zhao et al., “Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication,” JOURNAL OF VIROLOGY, vol. 98, no. 10, 2024.

@article{01JJKNGM63JEKCCPHXMADE8VQF,
  abstract     = {{Pseudorabies virus (PRV) utilizes multiple strategies to inhibit type I interferon (IFN-I) production and signaling to achieve innate immune evasion. Among several other functions, mitochondria serve as a crucial immune hub in the initiation of innate antiviral responses. It is currently unknown whether PRV inhibits innate immune responses by manipulating mitochondria. In this study, we found that PRV infection damages mitochondrial structure and function, as shown by mitochondrial membrane potential depolarization, reduction in mitochondrial numbers, and an imbalance in mitochondrial dynamics. In addition, PRV infection triggered PINK1-Parkin-mediated mitophagy to eliminate the impaired mitochondria, which resulted in a suppression of IFN-I production, thereby promoting viral replication. Furthermore, we found that mitophagy resulted in the degradation of the mitochondrial antiviral signaling protein, which is located on the mitochondrial outer membrane. In conclusion, the data of the current study indicate that PRV-induced mitophagy represents a previously uncharacterized PRV evasion mechanism of the IFN-I response, thereby promoting virus replication.IMPORTANCEPseudorabies virus (PRV), a pathogen that induces different disease symptoms and is often fatal in domestic animals and wildlife, has caused great economic losses to the swine industry. Since 2011, different PRV variant strains have emerged in Asia, against which current commercial vaccines may not always provide optimal protection in pigs. In addition, there are indications that some of these PRV variant strains may sporadically infect people. In the current study, we found that PRV infection causes mitochondria injury. This is associated with the induction of mitophagy to eliminate the damaged mitochondria, which results in suppressed antiviral interferon production and signaling. Hence, our study reveals a novel mechanism that is used by PRV to antagonize the antiviral host immune response, providing a theoretical basis that may contribute to the research toward and development of new vaccines and antiviral drugs.

Pseudorabies virus (PRV), a pathogen that induces different disease symptoms and is often fatal in domestic animals and wildlife, has caused great economic losses to the swine industry. Since 2011, different PRV variant strains have emerged in Asia, against which current commercial vaccines may not always provide optimal protection in pigs. In addition, there are indications that some of these PRV variant strains may sporadically infect people. In the current study, we found that PRV infection causes mitochondria injury. This is associated with the induction of mitophagy to eliminate the damaged mitochondria, which results in suppressed antiviral interferon production and signaling. Hence, our study reveals a novel mechanism that is used by PRV to antagonize the antiviral host immune response, providing a theoretical basis that may contribute to the research toward and development of new vaccines and antiviral drugs.}},
  articleno    = {{e01048-24}},
  author       = {{Zhao, Yuan and Ding, Chan and Zhu, Zhenbang and Wang, Wenqiang and Wen, Wei and Favoreel, Herman and Li, Xiangdong}},
  editor       = {{Cliffe, Anna Ruth}},
  issn         = {{0022-538X}},
  journal      = {{JOURNAL OF VIROLOGY}},
  keywords     = {{pseudorabies virus (PRV),mitochondria,mitophagy,MAVS,interferons production inhibition,MITOCHONDRIAL DYNAMICS,PROTEIN}},
  language     = {{eng}},
  number       = {{10}},
  pages        = {{17}},
  title        = {{Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication}},
  url          = {{http://doi.org/10.1128/jvi.01048-24}},
  volume       = {{98}},
  year         = {{2024}},
}

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Pseudorabies virus infection triggers mitophagy to dampen the interferon response and promote viral replication

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