Type I Interferon Signaling is Required for Oncostatin-M Driven Inflammatory Responses in Mouse Lung
Type I interferons (IFNs) consist of a group of structurally similar cytokines that play an integral role in regulating the immune response to combat lung infections. In certain models type I IFNs have also been associated with suppression of Th2-skewed immune and inflammatory responses. Transient p...
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| Veröffentlicht in: | Journal of interferon & cytokine research 2022-11, Vol.42 (11), p.568-579 |
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| creator | MacDonald, Kyle Botelho, Fernando Ashkar, Ali A. Richards, Carl D. |
| description | Type I interferons (IFNs) consist of a group of structurally similar cytokines that play an integral role in regulating the immune response to combat lung infections. In certain models type I IFNs have also been associated with suppression of Th2-skewed immune and inflammatory responses. Transient pulmonary overexpression of the gp130 cytokine Oncostatin M (OSM) by Adenovirus vector (AdOSM) induces a robust Th2-skewed cytokine/inflammatory profile in C57Bl/6 murine lungs. In this study we assessed type I IFN function in OSM-mediated inflammation in vivo using Ifnar1–/– C57Bl/6 mice and Ifnar1-deficient cells in vitro. Ifnar1–/– mice showed a significant reduction in AdOSM-induced histopathology (epithelial hyperplasia, alveolar septal wall thickening, cellular infiltration), and levels of IL-6 and chemokine protein (CXCL-1/KC and CCL24/eotaxin-2) in lungs compared with wild-type. Ifnar1–/– murine fibroblasts and human type I IFN receptor (Ifnar)-knockdown fibroblasts were also less responsive to OSM in STAT3 activation and cytokine production compared with Ifnar-sufficient cells in vitro. Exogenous type I IFN induced IL-6 responses in mouse and human fibroblasts and in combination with OSM further stimulated IL-6 production, suggesting a concerted action of type I IFNs and OSM. Taken together, these results demonstrate that cross-talk between IFNAR and OSM signaling enhances cell responses and modulates OSM-driven responses in lung inflammation. |
| doi_str_mv | 10.1089/jir.2022.0136 |
| format | Article |
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In certain models type I IFNs have also been associated with suppression of Th2-skewed immune and inflammatory responses. Transient pulmonary overexpression of the gp130 cytokine Oncostatin M (OSM) by Adenovirus vector (AdOSM) induces a robust Th2-skewed cytokine/inflammatory profile in C57Bl/6 murine lungs. In this study we assessed type I IFN function in OSM-mediated inflammation in vivo using Ifnar1–/– C57Bl/6 mice and Ifnar1-deficient cells in vitro. Ifnar1–/– mice showed a significant reduction in AdOSM-induced histopathology (epithelial hyperplasia, alveolar septal wall thickening, cellular infiltration), and levels of IL-6 and chemokine protein (CXCL-1/KC and CCL24/eotaxin-2) in lungs compared with wild-type. Ifnar1–/– murine fibroblasts and human type I IFN receptor (Ifnar)-knockdown fibroblasts were also less responsive to OSM in STAT3 activation and cytokine production compared with Ifnar-sufficient cells in vitro. Exogenous type I IFN induced IL-6 responses in mouse and human fibroblasts and in combination with OSM further stimulated IL-6 production, suggesting a concerted action of type I IFNs and OSM. Taken together, these results demonstrate that cross-talk between IFNAR and OSM signaling enhances cell responses and modulates OSM-driven responses in lung inflammation.</description><identifier>ISSN: 1079-9907</identifier><identifier>EISSN: 1557-7465</identifier><identifier>DOI: 10.1089/jir.2022.0136</identifier><language>eng</language><publisher>New Rochelle: Mary Ann Liebert, Inc</publisher><subject>Alveoli ; Bronchopulmonary infection ; Chemokines ; Cytokines ; Eotaxin ; Fibroblasts ; Glycoprotein gp130 ; Histopathology ; Hyperplasia ; Immune response ; Immune system ; In vivo methods and tests ; Inflammation ; Interferon ; Interleukin 6 ; Lungs ; Lymphocytes T ; Oncostatin M ; Signaling ; Stat3 protein ; Thickening</subject><ispartof>Journal of interferon & cytokine research, 2022-11, Vol.42 (11), p.568-579</ispartof><rights>Copyright Mary Ann Liebert, Inc. 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In certain models type I IFNs have also been associated with suppression of Th2-skewed immune and inflammatory responses. Transient pulmonary overexpression of the gp130 cytokine Oncostatin M (OSM) by Adenovirus vector (AdOSM) induces a robust Th2-skewed cytokine/inflammatory profile in C57Bl/6 murine lungs. In this study we assessed type I IFN function in OSM-mediated inflammation in vivo using Ifnar1–/– C57Bl/6 mice and Ifnar1-deficient cells in vitro. Ifnar1–/– mice showed a significant reduction in AdOSM-induced histopathology (epithelial hyperplasia, alveolar septal wall thickening, cellular infiltration), and levels of IL-6 and chemokine protein (CXCL-1/KC and CCL24/eotaxin-2) in lungs compared with wild-type. Ifnar1–/– murine fibroblasts and human type I IFN receptor (Ifnar)-knockdown fibroblasts were also less responsive to OSM in STAT3 activation and cytokine production compared with Ifnar-sufficient cells in vitro. Exogenous type I IFN induced IL-6 responses in mouse and human fibroblasts and in combination with OSM further stimulated IL-6 production, suggesting a concerted action of type I IFNs and OSM. Taken together, these results demonstrate that cross-talk between IFNAR and OSM signaling enhances cell responses and modulates OSM-driven responses in lung inflammation.</description><subject>Alveoli</subject><subject>Bronchopulmonary infection</subject><subject>Chemokines</subject><subject>Cytokines</subject><subject>Eotaxin</subject><subject>Fibroblasts</subject><subject>Glycoprotein gp130</subject><subject>Histopathology</subject><subject>Hyperplasia</subject><subject>Immune response</subject><subject>Immune system</subject><subject>In vivo methods and tests</subject><subject>Inflammation</subject><subject>Interferon</subject><subject>Interleukin 6</subject><subject>Lungs</subject><subject>Lymphocytes T</subject><subject>Oncostatin M</subject><subject>Signaling</subject><subject>Stat3 protein</subject><subject>Thickening</subject><issn>1079-9907</issn><issn>1557-7465</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2022</creationdate><recordtype>article</recordtype><recordid>eNpdkDtPwzAQgC0EEqUwsltiYUnxI4ntEZVXpVaVoMyR41wqV4md2glS_z0JMDHdSffd60PolpIFJVI9HGxYMMLYglCen6EZzTKRiDTPzsecCJUoRcQluorxQAjJJVMzVO1OHeAVXrkeQg3BO_xh90431u2xjfgdjoMNUOHaB7x1xsde99YlG_wU7Be4sbFudNvq3ofTSMfOuwgRW4c3foiA14PbX6OLWjcRbv7iHH2-PO-Wb8l6-7paPq4Tw5Tsk5TmhJaUG1HKTIDMTQkVUF6pNC81lyljKmNTQZYk5ZyyUpkaTKkyQ5jQfI7uf-d2wR8HiH3R2migabSD8ZiCCT7ukETyEb37hx78EMa_f6g8FzRNJyr5pUzwMQaoiy7YVodTQUkxOS9G58XkvJic8286XXQb</recordid><startdate>20221101</startdate><enddate>20221101</enddate><creator>MacDonald, Kyle</creator><creator>Botelho, Fernando</creator><creator>Ashkar, Ali A.</creator><creator>Richards, Carl D.</creator><general>Mary Ann Liebert, Inc</general><scope>AAYXX</scope><scope>CITATION</scope><scope>7QL</scope><scope>7T5</scope><scope>7T7</scope><scope>7TM</scope><scope>7U9</scope><scope>8FD</scope><scope>C1K</scope><scope>FR3</scope><scope>H94</scope><scope>K9.</scope><scope>M7N</scope><scope>P64</scope><scope>7X8</scope><orcidid>https://orcid.org/0000-0002-0081-2231</orcidid></search><sort><creationdate>20221101</creationdate><title>Type I Interferon Signaling is Required for Oncostatin-M Driven Inflammatory Responses in Mouse Lung</title><author>MacDonald, Kyle ; 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Exogenous type I IFN induced IL-6 responses in mouse and human fibroblasts and in combination with OSM further stimulated IL-6 production, suggesting a concerted action of type I IFNs and OSM. Taken together, these results demonstrate that cross-talk between IFNAR and OSM signaling enhances cell responses and modulates OSM-driven responses in lung inflammation.</abstract><cop>New Rochelle</cop><pub>Mary Ann Liebert, Inc</pub><doi>10.1089/jir.2022.0136</doi><tpages>12</tpages><orcidid>https://orcid.org/0000-0002-0081-2231</orcidid></addata></record> |
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| source | Alma/SFX Local Collection |
| subjects | Alveoli Bronchopulmonary infection Chemokines Cytokines Eotaxin Fibroblasts Glycoprotein gp130 Histopathology Hyperplasia Immune response Immune system In vivo methods and tests Inflammation Interferon Interleukin 6 Lungs Lymphocytes T Oncostatin M Signaling Stat3 protein Thickening |
| title | Type I Interferon Signaling is Required for Oncostatin-M Driven Inflammatory Responses in Mouse Lung |
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