Viperin binds STING and enhances the type-I interferon response following dsDNA detection

Keaton M. Crosse; Ebony A. Monson; Arti B. Dumbrepatil; Monique Smith; Yeu Yang Tseng; Kylie H. Van der Hoek; Peter A. Revill; Subir Saker; David C. Tscharke; E. Neil G Marsh; Michael R. Beard; Karla J. Helbig

doi:10.1111/imcb.12420

Viperin binds STING and enhances the type-I interferon response following dsDNA detection

Keaton M. Crosse, Ebony A. Monson, Arti B. Dumbrepatil, Monique Smith, Yeu Yang Tseng, Kylie H. Van der Hoek, Peter A. Revill, Subir Saker, David C. Tscharke, E. Neil G Marsh, Michael R. Beard, Karla J. Helbig^*

^*Corresponding author for this work

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

26 Citations (Scopus)

Abstract

Viperin is an interferon-inducible protein that is pivotal for eliciting an effective immune response against an array of diverse viral pathogens. Here we describe a mechanism of viperin’s broad antiviral activity by demonstrating the protein’s ability to synergistically enhance the innate immune dsDNA signaling pathway to limit viral infection. Viperin co-localized with the key signaling molecules of the innate immune dsDNA sensing pathway, STING and TBK1; binding directly to STING and inducing enhanced K63-linked polyubiquitination of TBK1. Subsequent analysis identified viperin’s necessity to bind the cytosolic iron-sulfur assembly component 2A, to prolong its enhancement of the type-I interferon response to aberrant dsDNA. Here we show that viperin facilitates the formation of a signaling enhanceosome, to coordinate efficient signal transduction following activation of the dsDNA signaling pathway, which results in an enhanced antiviral state. We also provide evidence for viperin’s radical SAM enzymatic activity to self-limit its immunomodulatory functions. These data further define viperin’s role as a positive regulator of innate immune signaling, offering a mechanism of viperin’s broad antiviral capacity.

Original language	English
Pages (from-to)	373-391
Number of pages	19
Journal	Immunology and Cell Biology
Volume	99
Issue number	4
DOIs	https://doi.org/10.1111/imcb.12420
Publication status	Published - Apr 2021

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title = "Viperin binds STING and enhances the type-I interferon response following dsDNA detection",

abstract = "Viperin is an interferon-inducible protein that is pivotal for eliciting an effective immune response against an array of diverse viral pathogens. Here we describe a mechanism of viperin{\textquoteright}s broad antiviral activity by demonstrating the protein{\textquoteright}s ability to synergistically enhance the innate immune dsDNA signaling pathway to limit viral infection. Viperin co-localized with the key signaling molecules of the innate immune dsDNA sensing pathway, STING and TBK1; binding directly to STING and inducing enhanced K63-linked polyubiquitination of TBK1. Subsequent analysis identified viperin{\textquoteright}s necessity to bind the cytosolic iron-sulfur assembly component 2A, to prolong its enhancement of the type-I interferon response to aberrant dsDNA. Here we show that viperin facilitates the formation of a signaling enhanceosome, to coordinate efficient signal transduction following activation of the dsDNA signaling pathway, which results in an enhanced antiviral state. We also provide evidence for viperin{\textquoteright}s radical SAM enzymatic activity to self-limit its immunomodulatory functions. These data further define viperin{\textquoteright}s role as a positive regulator of innate immune signaling, offering a mechanism of viperin{\textquoteright}s broad antiviral capacity.",

keywords = "CIA2A, STING, interferon, radical SAM enzyme, viperin",

author = "Crosse, {Keaton M.} and Monson, {Ebony A.} and Dumbrepatil, {Arti B.} and Monique Smith and Tseng, {Yeu Yang} and {Van der Hoek}, {Kylie H.} and Revill, {Peter A.} and Subir Saker and Tscharke, {David C.} and {G Marsh}, {E. Neil} and Beard, {Michael R.} and Helbig, {Karla J.}",

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year = "2021",

month = apr,

doi = "10.1111/imcb.12420",

language = "English",

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AU - Crosse, Keaton M.

AU - Monson, Ebony A.

AU - Dumbrepatil, Arti B.

AU - Smith, Monique

AU - Tseng, Yeu Yang

AU - Van der Hoek, Kylie H.

AU - Revill, Peter A.

AU - Saker, Subir

AU - Tscharke, David C.

AU - G Marsh, E. Neil

AU - Beard, Michael R.

AU - Helbig, Karla J.

PY - 2021/4

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N2 - Viperin is an interferon-inducible protein that is pivotal for eliciting an effective immune response against an array of diverse viral pathogens. Here we describe a mechanism of viperin’s broad antiviral activity by demonstrating the protein’s ability to synergistically enhance the innate immune dsDNA signaling pathway to limit viral infection. Viperin co-localized with the key signaling molecules of the innate immune dsDNA sensing pathway, STING and TBK1; binding directly to STING and inducing enhanced K63-linked polyubiquitination of TBK1. Subsequent analysis identified viperin’s necessity to bind the cytosolic iron-sulfur assembly component 2A, to prolong its enhancement of the type-I interferon response to aberrant dsDNA. Here we show that viperin facilitates the formation of a signaling enhanceosome, to coordinate efficient signal transduction following activation of the dsDNA signaling pathway, which results in an enhanced antiviral state. We also provide evidence for viperin’s radical SAM enzymatic activity to self-limit its immunomodulatory functions. These data further define viperin’s role as a positive regulator of innate immune signaling, offering a mechanism of viperin’s broad antiviral capacity.

AB - Viperin is an interferon-inducible protein that is pivotal for eliciting an effective immune response against an array of diverse viral pathogens. Here we describe a mechanism of viperin’s broad antiviral activity by demonstrating the protein’s ability to synergistically enhance the innate immune dsDNA signaling pathway to limit viral infection. Viperin co-localized with the key signaling molecules of the innate immune dsDNA sensing pathway, STING and TBK1; binding directly to STING and inducing enhanced K63-linked polyubiquitination of TBK1. Subsequent analysis identified viperin’s necessity to bind the cytosolic iron-sulfur assembly component 2A, to prolong its enhancement of the type-I interferon response to aberrant dsDNA. Here we show that viperin facilitates the formation of a signaling enhanceosome, to coordinate efficient signal transduction following activation of the dsDNA signaling pathway, which results in an enhanced antiviral state. We also provide evidence for viperin’s radical SAM enzymatic activity to self-limit its immunomodulatory functions. These data further define viperin’s role as a positive regulator of innate immune signaling, offering a mechanism of viperin’s broad antiviral capacity.

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Viperin binds STING and enhances the type-I interferon response following dsDNA detection

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