Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1

Autocrine priming of cells by small quantities of constitutively produced type I interferon (IFN) is a well-known phenomenon. In the absence of type I IFN priming, cells display attenuated responses to other cytokines, such as anti-viral protection in response to IFNγ. This phenomenon was proposed t...

Descripción completa

Detalles Bibliográficos
Autores principales: Gough, Daniel J., Messina, Nicole L., Hii, Linda, Gould, Jodee A., Sabapathy, Kanaga, Robertson, Ashley P. S., Trapani, Joseph A., Levy, David E., Hertzog, Paul J., Clarke, Christopher J. P., Johnstone, Ricky W.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2860501/
https://www.ncbi.nlm.nih.gov/pubmed/20436908
http://dx.doi.org/10.1371/journal.pbio.1000361
_version_ 1782180588243910656
author Gough, Daniel J.
Messina, Nicole L.
Hii, Linda
Gould, Jodee A.
Sabapathy, Kanaga
Robertson, Ashley P. S.
Trapani, Joseph A.
Levy, David E.
Hertzog, Paul J.
Clarke, Christopher J. P.
Johnstone, Ricky W.
author_facet Gough, Daniel J.
Messina, Nicole L.
Hii, Linda
Gould, Jodee A.
Sabapathy, Kanaga
Robertson, Ashley P. S.
Trapani, Joseph A.
Levy, David E.
Hertzog, Paul J.
Clarke, Christopher J. P.
Johnstone, Ricky W.
author_sort Gough, Daniel J.
collection PubMed
description Autocrine priming of cells by small quantities of constitutively produced type I interferon (IFN) is a well-known phenomenon. In the absence of type I IFN priming, cells display attenuated responses to other cytokines, such as anti-viral protection in response to IFNγ. This phenomenon was proposed to be because IFNα/β receptor1 (IFNAR1) is a component of the IFNγ receptor (IFNGR), but our new data are more consistent with a previously proposed model indicating that regulated expression of STAT1 may also play a critical role in the priming process. Initially, we noticed that DNA binding activity of STAT1 was attenuated in c-Jun (−/−) fibroblasts because they expressed lower levels of STAT1 than wild-type cells. However, expression of STAT1 was rescued by culturing c-Jun (−/−) fibroblasts in media conditioned by wild-type fibroblasts suggesting they secreted a STAT1-inducing factor. The STAT1-inducing factor in fibroblast-conditioned media was IFNβ, as it was inhibited by antibodies to IFNAR1, or when IFNβ expression was knocked down in wild-type cells. IFNAR1(−/−) fibroblasts, which cannot respond to this priming, also expressed reduced levels of STAT1, which correlated with their poor responses to IFNγ. The lack of priming in IFNAR1(−/−) fibroblasts was compensated by over-expression of STAT1, which rescued molecular responses to IFNγ and restored the ability of IFNγ to induce protective anti-viral immunity. This study provides a comprehensive description of the molecular events involved in priming by type I IFN. Adding to the previous working model that proposed an interaction between type I and II IFN receptors, our work and that of others demonstrates that type I IFN primes IFNγ-mediated immune responses by regulating expression of STAT1. This may also explain how type I IFN can additionally prime cells to respond to a range of other cytokines that use STAT1 (e.g., IL-6, M-CSF, IL-10) and suggests a potential mechanism for the changing levels of STAT1 expression observed during viral infection.
format Text
id pubmed-2860501
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-28605012010-04-30 Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1 Gough, Daniel J. Messina, Nicole L. Hii, Linda Gould, Jodee A. Sabapathy, Kanaga Robertson, Ashley P. S. Trapani, Joseph A. Levy, David E. Hertzog, Paul J. Clarke, Christopher J. P. Johnstone, Ricky W. PLoS Biol Research Article Autocrine priming of cells by small quantities of constitutively produced type I interferon (IFN) is a well-known phenomenon. In the absence of type I IFN priming, cells display attenuated responses to other cytokines, such as anti-viral protection in response to IFNγ. This phenomenon was proposed to be because IFNα/β receptor1 (IFNAR1) is a component of the IFNγ receptor (IFNGR), but our new data are more consistent with a previously proposed model indicating that regulated expression of STAT1 may also play a critical role in the priming process. Initially, we noticed that DNA binding activity of STAT1 was attenuated in c-Jun (−/−) fibroblasts because they expressed lower levels of STAT1 than wild-type cells. However, expression of STAT1 was rescued by culturing c-Jun (−/−) fibroblasts in media conditioned by wild-type fibroblasts suggesting they secreted a STAT1-inducing factor. The STAT1-inducing factor in fibroblast-conditioned media was IFNβ, as it was inhibited by antibodies to IFNAR1, or when IFNβ expression was knocked down in wild-type cells. IFNAR1(−/−) fibroblasts, which cannot respond to this priming, also expressed reduced levels of STAT1, which correlated with their poor responses to IFNγ. The lack of priming in IFNAR1(−/−) fibroblasts was compensated by over-expression of STAT1, which rescued molecular responses to IFNγ and restored the ability of IFNγ to induce protective anti-viral immunity. This study provides a comprehensive description of the molecular events involved in priming by type I IFN. Adding to the previous working model that proposed an interaction between type I and II IFN receptors, our work and that of others demonstrates that type I IFN primes IFNγ-mediated immune responses by regulating expression of STAT1. This may also explain how type I IFN can additionally prime cells to respond to a range of other cytokines that use STAT1 (e.g., IL-6, M-CSF, IL-10) and suggests a potential mechanism for the changing levels of STAT1 expression observed during viral infection. Public Library of Science 2010-04-27 /pmc/articles/PMC2860501/ /pubmed/20436908 http://dx.doi.org/10.1371/journal.pbio.1000361 Text en Gough et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Gough, Daniel J.
Messina, Nicole L.
Hii, Linda
Gould, Jodee A.
Sabapathy, Kanaga
Robertson, Ashley P. S.
Trapani, Joseph A.
Levy, David E.
Hertzog, Paul J.
Clarke, Christopher J. P.
Johnstone, Ricky W.
Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title_full Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title_fullStr Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title_full_unstemmed Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title_short Functional Crosstalk between Type I and II Interferon through the Regulated Expression of STAT1
title_sort functional crosstalk between type i and ii interferon through the regulated expression of stat1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2860501/
https://www.ncbi.nlm.nih.gov/pubmed/20436908
http://dx.doi.org/10.1371/journal.pbio.1000361
work_keys_str_mv AT goughdanielj functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT messinanicolel functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT hiilinda functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT gouldjodeea functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT sabapathykanaga functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT robertsonashleyps functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT trapanijosepha functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT levydavide functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT hertzogpaulj functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT clarkechristopherjp functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1
AT johnstonerickyw functionalcrosstalkbetweentypeiandiiinterferonthroughtheregulatedexpressionofstat1

Ejemplares similares