Autophagy Protects against Sindbis Virus Infection of the Central Nervous System

Anthony Orvedahl; Sarah MacPherson; Rhea Sumpter; Zsolt Tallóczy; Zhongju Zou; Beth Levine

doi:10.1016/j.chom.2010.01.007

Autophagy Protects against Sindbis Virus Infection of the Central Nervous System

Anthony Orvedahl, Sarah MacPherson, Rhea Sumpter, Zsolt Tallóczy, Zhongju Zou, Beth Levine

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

441 Scopus citations

Abstract

Autophagy functions in antiviral immunity. However, the ability of endogenous autophagy genes to protect against viral disease in vertebrates remains to be causally established. Here, we report that the autophagy gene Atg5 function is critical for protection against lethal Sindbis virus (SIN) infection of the mouse central nervous system. Inactivating Atg5 in SIN-infected neurons results in delayed clearance of viral proteins, increased accumulation of the cellular p62 adaptor protein, and increased cell death in neurons, but the levels of viral replication remain unaltered. In vitro, p62 interacts with SIN capsid protein, and genetic knockdown of p62 blocks the targeting of viral capsid to autophagosomes. Moreover, p62 or autophagy gene knockdown increases viral capsid accumulation and accelerates virus-induced cell death without affecting virus replication. These results suggest a function for autophagy in mammalian antiviral defense: a cell-autonomous mechanism in which p62 adaptor-mediated autophagic viral protein clearance promotes cell survival.

Original language	English (US)
Pages (from-to)	115-127
Number of pages	13
Journal	Cell Host and Microbe
Volume	7
Issue number	2
DOIs	https://doi.org/10.1016/j.chom.2010.01.007
State	Published - Feb 18 2010

Keywords

MICROBIO
MOLIMMUNO
MOLNEURO

ASJC Scopus subject areas

Parasitology
Microbiology
Virology

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10.1016/j.chom.2010.01.007

Cite this

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title = "Autophagy Protects against Sindbis Virus Infection of the Central Nervous System",

abstract = "Autophagy functions in antiviral immunity. However, the ability of endogenous autophagy genes to protect against viral disease in vertebrates remains to be causally established. Here, we report that the autophagy gene Atg5 function is critical for protection against lethal Sindbis virus (SIN) infection of the mouse central nervous system. Inactivating Atg5 in SIN-infected neurons results in delayed clearance of viral proteins, increased accumulation of the cellular p62 adaptor protein, and increased cell death in neurons, but the levels of viral replication remain unaltered. In vitro, p62 interacts with SIN capsid protein, and genetic knockdown of p62 blocks the targeting of viral capsid to autophagosomes. Moreover, p62 or autophagy gene knockdown increases viral capsid accumulation and accelerates virus-induced cell death without affecting virus replication. These results suggest a function for autophagy in mammalian antiviral defense: a cell-autonomous mechanism in which p62 adaptor-mediated autophagic viral protein clearance promotes cell survival.",

keywords = "MICROBIO, MOLIMMUNO, MOLNEURO",

author = "Anthony Orvedahl and Sarah MacPherson and Rhea Sumpter and Zsolt Tall{\'o}czy and Zhongju Zou and Beth Levine",

note = "Funding Information: We thank Diane Griffin, David Leib, Margaret MacDonald, Noboru Mizushima, Victor Stollar, and Tamotsu Yoshimori for providing critical reagents. We thank Abhijit Bugde and Kate Luby-Phelps for assistance with live cell imaging and Laurie Mueller for assistance with electron microscopy. This work was supported by the Ellison Medical Foundation Senior Scholars Award in Infectious Diseases (B.L.), NIH RO1 AI151367 (B.L.), and NIH T32 AI007520 (A.O.). ",

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language = "English (US)",

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AU - Orvedahl, Anthony

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AU - Tallóczy, Zsolt

AU - Zou, Zhongju

AU - Levine, Beth

N1 - Funding Information: We thank Diane Griffin, David Leib, Margaret MacDonald, Noboru Mizushima, Victor Stollar, and Tamotsu Yoshimori for providing critical reagents. We thank Abhijit Bugde and Kate Luby-Phelps for assistance with live cell imaging and Laurie Mueller for assistance with electron microscopy. This work was supported by the Ellison Medical Foundation Senior Scholars Award in Infectious Diseases (B.L.), NIH RO1 AI151367 (B.L.), and NIH T32 AI007520 (A.O.).

PY - 2010/2/18

Y1 - 2010/2/18

N2 - Autophagy functions in antiviral immunity. However, the ability of endogenous autophagy genes to protect against viral disease in vertebrates remains to be causally established. Here, we report that the autophagy gene Atg5 function is critical for protection against lethal Sindbis virus (SIN) infection of the mouse central nervous system. Inactivating Atg5 in SIN-infected neurons results in delayed clearance of viral proteins, increased accumulation of the cellular p62 adaptor protein, and increased cell death in neurons, but the levels of viral replication remain unaltered. In vitro, p62 interacts with SIN capsid protein, and genetic knockdown of p62 blocks the targeting of viral capsid to autophagosomes. Moreover, p62 or autophagy gene knockdown increases viral capsid accumulation and accelerates virus-induced cell death without affecting virus replication. These results suggest a function for autophagy in mammalian antiviral defense: a cell-autonomous mechanism in which p62 adaptor-mediated autophagic viral protein clearance promotes cell survival.

AB - Autophagy functions in antiviral immunity. However, the ability of endogenous autophagy genes to protect against viral disease in vertebrates remains to be causally established. Here, we report that the autophagy gene Atg5 function is critical for protection against lethal Sindbis virus (SIN) infection of the mouse central nervous system. Inactivating Atg5 in SIN-infected neurons results in delayed clearance of viral proteins, increased accumulation of the cellular p62 adaptor protein, and increased cell death in neurons, but the levels of viral replication remain unaltered. In vitro, p62 interacts with SIN capsid protein, and genetic knockdown of p62 blocks the targeting of viral capsid to autophagosomes. Moreover, p62 or autophagy gene knockdown increases viral capsid accumulation and accelerates virus-induced cell death without affecting virus replication. These results suggest a function for autophagy in mammalian antiviral defense: a cell-autonomous mechanism in which p62 adaptor-mediated autophagic viral protein clearance promotes cell survival.

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Autophagy Protects against Sindbis Virus Infection of the Central Nervous System

Abstract

Keywords

ASJC Scopus subject areas

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