Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines
Investigating the relationships between critical influenza viral mutations contributing to increased virulence and host expression factors will shed light on the process of severe pathogenesis from the systems biology perspective. We previously generated a mouse-adapted, highly virulent influenza (H...
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sg-ntu-dr.10356-1000192020-05-28T07:17:31Z Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines Ivan, Fransiskus X. Rajapakse, Jagath C. Welsch, Roy E. Rozen, Steve G. Narasaraju, T. Xiong, Gordon M. Engelward, Bevin P. Chow, Vincent T. K. School of Computer Engineering Bioinformatics Research Centre DRNTU::Engineering::Computer science and engineering Investigating the relationships between critical influenza viral mutations contributing to increased virulence and host expression factors will shed light on the process of severe pathogenesis from the systems biology perspective. We previously generated a mouse-adapted, highly virulent influenza (HVI) virus through serial lung-to-lung passaging of a human influenza H3N2 virus strain that causes low virulent influenza (LVI) in murine lungs. This HVI virus is characterized by enhanced replication kinetics, severe lung injury, and systemic spread to major organs. Our gene microarray investigations compared the host transcriptomic responses of murine lungs to LVI virus and its HVI descendant at 12, 48, and 96 h following infection. More intense expression of genes associated with cytokine activity, type 1 interferon response, and apoptosis was evident in HVI at all time-points. We highlighted dysregulation of the TREM1 signaling pathway (an amplifier of cytokine production) that is likely to be upregulated in infiltrating neutrophils in HVI-infected lungs. The cytokine gene expression changes were corroborated by elevated levels of multiple cytokine and chemokine proteins in the bronchoalveolar lavage fluid of infected mice, especially at 12 h post-infection. Concomitantly, the downregulation of genes that mediate proliferative, developmental, and metabolic processes likely contributed to the lethality of HVI as well as lack of lung repair. Overall, our comparative transcriptomic study provided insights into key host factors that influence the dynamics, pathogenesis, and outcome of severe influenza. 2013-10-04T07:22:24Z 2019-12-06T20:15:11Z 2013-10-04T07:22:24Z 2019-12-06T20:15:11Z 2011 2011 Journal Article Ivan, F. X., Rajapakse, J. C., Welsch, R. E., Rozen, S. G., Narasaraju, T., Xiong, G. M., et al. (2011). Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines. Functional & Integrative Genomics, 12(1), 105-117. https://hdl.handle.net/10356/100019 http://hdl.handle.net/10220/16283 10.1007/s10142-011-0247-y en Functional & integrative genomics |
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DRNTU::Engineering::Computer science and engineering Ivan, Fransiskus X. Rajapakse, Jagath C. Welsch, Roy E. Rozen, Steve G. Narasaraju, T. Xiong, Gordon M. Engelward, Bevin P. Chow, Vincent T. K. Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
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Investigating the relationships between critical influenza viral mutations contributing to increased virulence and host expression factors will shed light on the process of severe pathogenesis from the systems biology perspective. We previously generated a mouse-adapted, highly virulent influenza (HVI) virus through serial lung-to-lung passaging of a human influenza H3N2 virus strain that causes low virulent influenza (LVI) in murine lungs. This HVI virus is characterized by enhanced replication kinetics, severe lung injury, and systemic spread to major organs. Our gene microarray investigations compared the host transcriptomic responses of murine lungs to LVI virus and its HVI descendant at 12, 48, and 96 h following infection. More intense expression of genes associated with cytokine activity, type 1 interferon response, and apoptosis was evident in HVI at all time-points. We highlighted dysregulation of the TREM1 signaling pathway (an amplifier of cytokine production) that is likely to be upregulated in infiltrating neutrophils in HVI-infected lungs. The cytokine gene expression changes were corroborated by elevated levels of multiple cytokine and chemokine proteins in the bronchoalveolar lavage fluid of infected mice, especially at 12 h post-infection. Concomitantly, the downregulation of genes that mediate proliferative, developmental, and metabolic processes likely contributed to the lethality of HVI as well as lack of lung repair. Overall, our comparative transcriptomic study provided insights into key host factors that influence the dynamics, pathogenesis, and outcome of severe influenza. |
| author2 |
School of Computer Engineering |
| author_facet |
School of Computer Engineering Ivan, Fransiskus X. Rajapakse, Jagath C. Welsch, Roy E. Rozen, Steve G. Narasaraju, T. Xiong, Gordon M. Engelward, Bevin P. Chow, Vincent T. K. |
| format |
Article |
| author |
Ivan, Fransiskus X. Rajapakse, Jagath C. Welsch, Roy E. Rozen, Steve G. Narasaraju, T. Xiong, Gordon M. Engelward, Bevin P. Chow, Vincent T. K. |
| author_sort |
Ivan, Fransiskus X. |
| title |
Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
| title_short |
Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
| title_full |
Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
| title_fullStr |
Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
| title_full_unstemmed |
Differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza H3N2 viruses reveal dysregulation of TREM1 signaling, cytokines, and chemokines |
| title_sort |
differential pulmonary transcriptomic profiles in murine lungs infected with low and highly virulent influenza h3n2 viruses reveal dysregulation of trem1 signaling, cytokines, and chemokines |
| publishDate |
2013 |
| url |
https://hdl.handle.net/10356/100019 http://hdl.handle.net/10220/16283 |
| _version_ |
1681059531483774976 |