Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers
Background: During respiratory syncytial virus (RSV) infection filamentous virus particles are formed on the cell surface. Although the virus infectivity remains cell-associated, low levels of cell-free virus is detected during advanced infection. It is currently unclear if this cell-free virus infe...
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sg-ntu-dr.10356-823532023-02-28T17:03:20Z Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers Huong, Tra Nguyen Ravi, Laxmi Iyer Tan, Boon Huan Sugrue, Richard J. School of Biological Sciences Biological Sciences Background: During respiratory syncytial virus (RSV) infection filamentous virus particles are formed on the cell surface. Although the virus infectivity remains cell-associated, low levels of cell-free virus is detected during advanced infection. It is currently unclear if this cell-free virus infectivity is due to a low-efficiency specific cell-release mechanism, or if it arises due to mechanical breakage following virus-induced cell damage at the advanced stage of infection. Understanding the origin of this cell-free virus is a prerequisite for understanding the mechanism of RSV transmission in permissive cells. In this study we describe a detailed examination of RSV transmission in permissive HEp2 cell monolayers. Methods: HEp2 cell monolayers were infected with RSV using a multiplicity of infection of 0.0002, and the course of infection monitored over 5 days. The progression of the virus infection within the cell monolayers was performed using bright-field microscopy to visualise the cell monolayer and immunofluorescence microscopy to detect virus-infected cells. The cell-associated and cell-free virus infectivity were determined by virus plaque assay, and the virus-induced cell cytotoxicity determined by measuring cell membrane permeability and cellular DNA fragmentation. Results: At 2 days-post infection (dpi), large clusters of virus-infected cells could be detected indicating localised transmission in the cell monolayer, and during this stage we failed to detect either cell-free virus or cell cytotoxicity. At 3 dpi the presence of much larger infected cell clusters correlated with the begining of virus-induced changes in cell permeability. The presence of cell-free virus correlated with continued increase in cell permeability and cytotoxicity at 4 and 5 dpi. At 5 dpi extensive cell damage, syncytial formation, and increased cellular DNA fragmentation was noted. However, even at 5 dpi the cell-free virus constituted less than 1 % of the total virus infectivity. Conclusions: Our data supports a model of RSV transmission that initially involves the localised cell-to-cell spread of virus particles within the HEp2 cell monolayer. However, low levels of cell free-virus infectivity was observed at the advanced stages of infection, which correlated with a general loss in cell monolayer integrity due to virus-induced cytotoxicity. Published version 2016-02-03T08:29:01Z 2019-12-06T14:53:56Z 2016-02-03T08:29:01Z 2019-12-06T14:53:56Z 2016 Journal Article Huong, T. N., Ravi, L. I., Tan, B. H., & Sugrue, R. J. (2016). Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers. Virology Journal, 13, 12-. 1743-422X https://hdl.handle.net/10356/82353 http://hdl.handle.net/10220/39945 10.1186/s12985-016-0467-9 26790623 en Virology Journal © 2016 Huong et al. Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated. 17 p. application/pdf |
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Biological Sciences Huong, Tra Nguyen Ravi, Laxmi Iyer Tan, Boon Huan Sugrue, Richard J. Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| description |
Background: During respiratory syncytial virus (RSV) infection filamentous virus particles are formed on the cell surface. Although the virus infectivity remains cell-associated, low levels of cell-free virus is detected during advanced infection. It is currently unclear if this cell-free virus infectivity is due to a low-efficiency specific cell-release mechanism, or if it arises due to mechanical breakage following virus-induced cell damage at the advanced stage of infection. Understanding the origin of this cell-free virus is a prerequisite for understanding the mechanism of RSV transmission in permissive cells. In this study we describe a detailed examination of RSV transmission in permissive HEp2 cell monolayers.
Methods: HEp2 cell monolayers were infected with RSV using a multiplicity of infection of 0.0002, and the course of infection monitored over 5 days. The progression of the virus infection within the cell monolayers was performed using bright-field microscopy to visualise the cell monolayer and immunofluorescence microscopy to detect virus-infected cells. The cell-associated and cell-free virus infectivity were determined by virus plaque assay, and the virus-induced cell cytotoxicity determined by measuring cell membrane permeability and cellular DNA fragmentation.
Results: At 2 days-post infection (dpi), large clusters of virus-infected cells could be detected indicating localised transmission in the cell monolayer, and during this stage we failed to detect either cell-free virus or cell cytotoxicity. At 3 dpi the presence of much larger infected cell clusters correlated with the begining of virus-induced changes in cell permeability. The presence of cell-free virus correlated with continued increase in cell permeability and cytotoxicity at 4 and 5 dpi. At 5 dpi extensive cell damage, syncytial formation, and increased cellular DNA fragmentation was noted. However, even at 5 dpi the cell-free virus constituted less than 1 % of the total virus infectivity.
Conclusions: Our data supports a model of RSV transmission that initially involves the localised cell-to-cell spread of virus particles within the HEp2 cell monolayer. However, low levels of cell free-virus infectivity was observed at the advanced stages of infection, which correlated with a general loss in cell monolayer integrity due to virus-induced cytotoxicity. |
| author2 |
School of Biological Sciences |
| author_facet |
School of Biological Sciences Huong, Tra Nguyen Ravi, Laxmi Iyer Tan, Boon Huan Sugrue, Richard J. |
| format |
Article |
| author |
Huong, Tra Nguyen Ravi, Laxmi Iyer Tan, Boon Huan Sugrue, Richard J. |
| author_sort |
Huong, Tra Nguyen |
| title |
Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| title_short |
Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| title_full |
Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| title_fullStr |
Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| title_full_unstemmed |
Evidence for a biphasic mode of respiratory syncytial virus transmission in permissive HEp2 cell monolayers |
| title_sort |
evidence for a biphasic mode of respiratory syncytial virus transmission in permissive hep2 cell monolayers |
| publishDate |
2016 |
| url |
https://hdl.handle.net/10356/82353 http://hdl.handle.net/10220/39945 |
| _version_ |
1759854468408541184 |