Type i interferons link viral infection to enhanced epithelial turnover and repair

Lulu Sun; Hiroyuki Miyoshi; Sofia Origanti; Timothy J. Nice; Alexandra C. Barger; Nicholas A. Manieri; Leslie A. Fogel; Anthony R. French; David Piwnica-Worms; Helen Piwnica-Worms; Herbert W. Virgin; Deborah J. Lenschow; Thaddeus S. Stappenbeck

doi:10.1016/j.chom.2014.11.004

Type i interferons link viral infection to enhanced epithelial turnover and repair

Lulu Sun, Hiroyuki Miyoshi, Sofia Origanti, Timothy J. Nice, Alexandra C. Barger, Nicholas A. Manieri, Leslie A. Fogel, Anthony R. French, David Piwnica-Worms, Helen Piwnica-Worms, Herbert W. Virgin, Deborah J. Lenschow, Thaddeus S. Stappenbeck

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

72 Scopus citations

Abstract

The host immune system functions constantly to maintain chronic commensal and pathogenic organisms in check. The consequences of these immune responses on host physiology are as yet unexplored, and may have long-term implications in health and disease. We show that chronic viral infection increases epithelial turnover in multiple tissues, and the antiviral cytokines type I interferons (IFNs) mediate this response. Using a murine model with persistently elevated type I IFNs in the absence of exogenous viral infection, the Irgm1^-/- mouse, we demonstrate that type I IFNs act through nonepithelial cells, including macrophages, to promote increased epithelial turnover and wound repair. Downstream of type I IFN signaling, the highly related IFN-stimulated genes Apolipoprotein L9a and b activate epithelial proliferation through ERK activation. Our findings demonstrate that the host immune response to chronic viral infection has systemic effects on epithelial turnover through a myeloid-epithelial circuit.

Original language	English (US)
Pages (from-to)	85-97
Number of pages	13
Journal	Cell Host and Microbe
Volume	17
Issue number	1
DOIs	https://doi.org/10.1016/j.chom.2014.11.004
State	Published - Jan 14 2015
Externally published	Yes

ASJC Scopus subject areas

Parasitology
Microbiology
Virology

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Sun, L., Miyoshi, H., Origanti, S., Nice, T. J., Barger, A. C., Manieri, N. A., Fogel, L. A., French, A. R., Piwnica-Worms, D., Piwnica-Worms, H., Virgin, H. W., Lenschow, D. J., & Stappenbeck, T. S. (2015). Type i interferons link viral infection to enhanced epithelial turnover and repair. Cell Host and Microbe, 17(1), 85-97. https://doi.org/10.1016/j.chom.2014.11.004

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abstract = "The host immune system functions constantly to maintain chronic commensal and pathogenic organisms in check. The consequences of these immune responses on host physiology are as yet unexplored, and may have long-term implications in health and disease. We show that chronic viral infection increases epithelial turnover in multiple tissues, and the antiviral cytokines type I interferons (IFNs) mediate this response. Using a murine model with persistently elevated type I IFNs in the absence of exogenous viral infection, the Irgm1-/- mouse, we demonstrate that type I IFNs act through nonepithelial cells, including macrophages, to promote increased epithelial turnover and wound repair. Downstream of type I IFN signaling, the highly related IFN-stimulated genes Apolipoprotein L9a and b activate epithelial proliferation through ERK activation. Our findings demonstrate that the host immune response to chronic viral infection has systemic effects on epithelial turnover through a myeloid-epithelial circuit.",

author = "Lulu Sun and Hiroyuki Miyoshi and Sofia Origanti and Nice, {Timothy J.} and Barger, {Alexandra C.} and Manieri, {Nicholas A.} and Fogel, {Leslie A.} and French, {Anthony R.} and David Piwnica-Worms and Helen Piwnica-Worms and Virgin, {Herbert W.} and Lenschow, {Deborah J.} and Stappenbeck, {Thaddeus S.}",

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AU - Sun, Lulu

AU - Miyoshi, Hiroyuki

AU - Origanti, Sofia

AU - Nice, Timothy J.

AU - Barger, Alexandra C.

AU - Manieri, Nicholas A.

AU - Fogel, Leslie A.

AU - French, Anthony R.

AU - Piwnica-Worms, David

AU - Piwnica-Worms, Helen

AU - Virgin, Herbert W.

AU - Lenschow, Deborah J.

AU - Stappenbeck, Thaddeus S.

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N2 - The host immune system functions constantly to maintain chronic commensal and pathogenic organisms in check. The consequences of these immune responses on host physiology are as yet unexplored, and may have long-term implications in health and disease. We show that chronic viral infection increases epithelial turnover in multiple tissues, and the antiviral cytokines type I interferons (IFNs) mediate this response. Using a murine model with persistently elevated type I IFNs in the absence of exogenous viral infection, the Irgm1-/- mouse, we demonstrate that type I IFNs act through nonepithelial cells, including macrophages, to promote increased epithelial turnover and wound repair. Downstream of type I IFN signaling, the highly related IFN-stimulated genes Apolipoprotein L9a and b activate epithelial proliferation through ERK activation. Our findings demonstrate that the host immune response to chronic viral infection has systemic effects on epithelial turnover through a myeloid-epithelial circuit.

AB - The host immune system functions constantly to maintain chronic commensal and pathogenic organisms in check. The consequences of these immune responses on host physiology are as yet unexplored, and may have long-term implications in health and disease. We show that chronic viral infection increases epithelial turnover in multiple tissues, and the antiviral cytokines type I interferons (IFNs) mediate this response. Using a murine model with persistently elevated type I IFNs in the absence of exogenous viral infection, the Irgm1-/- mouse, we demonstrate that type I IFNs act through nonepithelial cells, including macrophages, to promote increased epithelial turnover and wound repair. Downstream of type I IFN signaling, the highly related IFN-stimulated genes Apolipoprotein L9a and b activate epithelial proliferation through ERK activation. Our findings demonstrate that the host immune response to chronic viral infection has systemic effects on epithelial turnover through a myeloid-epithelial circuit.

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Type i interferons link viral infection to enhanced epithelial turnover and repair

Abstract

ASJC Scopus subject areas

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