MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy
Abstract MX2 is an interferon inducible gene that is mostly known for its antiviral activity. We have previously demonstrated that MX2 is also associated with the tumorigenesis process in melanoma. However, it remains unknown which molecular mechanisms are regulated by MX2 in response to interferon...
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doaj-7baa4dc159db4d9e97171dddd62a00402021-04-08T04:25:01ZengWileyCancer Medicine2045-76342021-04-011082840285410.1002/cam4.3846MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapyMarina Juraleviciute0Jérémie Nsengimana1Julia Newton‐Bishop2Gert J. Hendriks3Ana Slipicevic4Department of Pathology Oslo University Hospital Oslo NorwayFaculty of Medical Sciences Population Health Sciences InstituteNewcastle University Newcastle upon Tyne UKDivision of Haematology and Immunology Institute of Medical Research at St James'sUniversity of Leeds Leeds UKDepartment of Cell and Molecular Biology Karolinska Institutet Stockholm SwedenDepartment of Pathology Oslo University Hospital Oslo NorwayAbstract MX2 is an interferon inducible gene that is mostly known for its antiviral activity. We have previously demonstrated that MX2 is also associated with the tumorigenesis process in melanoma. However, it remains unknown which molecular mechanisms are regulated by MX2 in response to interferon signaling in this disease. Here, we report that MX2 is necessary for the establishment of an interferon‐induced transcriptional profile partially through regulation of STAT1 phosphorylation and other interferon‐related downstream factors, including proapoptotic tumor suppressor XAF1. MX2 and XAF1 expression tightly correlate in both cultured melanoma cell lines and in patient‐derived primary and metastatic tumors, where they also are significantly related with survival. MX2 mediates IFN growth‐inhibitory signals in both XAF1 dependent and independent ways and in a cell type and context‐dependent manner. Higher MX2 expression renders melanoma cells more sensitive to targeted therapy drugs such as vemurafenib and trametinib; however, this effect is XAF1 independent. In summary, we uncovered a new mechanism in the complex regulation of interferon signaling in melanoma that can influence both survival and response to therapy.https://doi.org/10.1002/cam4.3846melanoma‐specific survivalMX2STAT1 phosphorylationXAF1 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Marina Juraleviciute Jérémie Nsengimana Julia Newton‐Bishop Gert J. Hendriks Ana Slipicevic |
spellingShingle |
Marina Juraleviciute Jérémie Nsengimana Julia Newton‐Bishop Gert J. Hendriks Ana Slipicevic MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy Cancer Medicine melanoma‐specific survival MX2 STAT1 phosphorylation XAF1 |
author_facet |
Marina Juraleviciute Jérémie Nsengimana Julia Newton‐Bishop Gert J. Hendriks Ana Slipicevic |
author_sort |
Marina Juraleviciute |
title |
MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy |
title_short |
MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy |
title_full |
MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy |
title_fullStr |
MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy |
title_full_unstemmed |
MX2 mediates establishment of interferon response profile, regulates XAF1, and can sensitize melanoma cells to targeted therapy |
title_sort |
mx2 mediates establishment of interferon response profile, regulates xaf1, and can sensitize melanoma cells to targeted therapy |
publisher |
Wiley |
series |
Cancer Medicine |
issn |
2045-7634 |
publishDate |
2021-04-01 |
description |
Abstract MX2 is an interferon inducible gene that is mostly known for its antiviral activity. We have previously demonstrated that MX2 is also associated with the tumorigenesis process in melanoma. However, it remains unknown which molecular mechanisms are regulated by MX2 in response to interferon signaling in this disease. Here, we report that MX2 is necessary for the establishment of an interferon‐induced transcriptional profile partially through regulation of STAT1 phosphorylation and other interferon‐related downstream factors, including proapoptotic tumor suppressor XAF1. MX2 and XAF1 expression tightly correlate in both cultured melanoma cell lines and in patient‐derived primary and metastatic tumors, where they also are significantly related with survival. MX2 mediates IFN growth‐inhibitory signals in both XAF1 dependent and independent ways and in a cell type and context‐dependent manner. Higher MX2 expression renders melanoma cells more sensitive to targeted therapy drugs such as vemurafenib and trametinib; however, this effect is XAF1 independent. In summary, we uncovered a new mechanism in the complex regulation of interferon signaling in melanoma that can influence both survival and response to therapy. |
topic |
melanoma‐specific survival MX2 STAT1 phosphorylation XAF1 |
url |
https://doi.org/10.1002/cam4.3846 |
work_keys_str_mv |
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