High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection

Viruses modulate a number of host biological responses including the cell cycle to favor their replication. In this study, we developed a high-content imaging (HCI) assay to measure DNA content and identify different phases of the cell cycle. We then investigated the potential effects of cell cycle...

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Main Authors: Sina Bavari, Rekha G. Panchal, Julie P. Tran, Rajini Mudhasani, Cary Retterer, Jacqueline G. Benko, Krishna P. Kota
Format: Article
Language:English
Published: MDPI AG 2012-09-01
Series:Viruses
Subjects:
Online Access:http://www.mdpi.com/1999-4915/4/10/1865
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spelling doaj-ce00f3581b8441bb8cbf68d5a6792e2b2020-11-24T23:52:58ZengMDPI AGViruses1999-49152012-09-014101865187710.3390/v4101865High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus InfectionSina BavariRekha G. PanchalJulie P. TranRajini MudhasaniCary RettererJacqueline G. BenkoKrishna P. KotaViruses modulate a number of host biological responses including the cell cycle to favor their replication. In this study, we developed a high-content imaging (HCI) assay to measure DNA content and identify different phases of the cell cycle. We then investigated the potential effects of cell cycle arrest on Ebola virus (EBOV) infection. Cells arrested in G1 phase by serum starvation or G1/S phase using aphidicolin or G2/M phase using nocodazole showed much reduced EBOV infection compared to the untreated control. Release of cells from serum starvation or aphidicolin block resulted in a time-dependent increase in the percentage of EBOV infected cells. The effect of EBOV infection on cell cycle progression was found to be cell-type dependent. Infection of asynchronous MCF-10A cells with EBOV resulted in a reduced number of cells in G2/M phase with concomitant increase of cells in G1 phase. However, these effects were not observed in HeLa or A549 cells. Together, our studies suggest that EBOV requires actively proliferating cells for efficient replication. Furthermore, multiplexing of HCI based assays to detect viral infection, cell cycle status and other phenotypic changes in a single cell population will provide useful information during screening campaigns using siRNA and small molecule therapeutics.http://www.mdpi.com/1999-4915/4/10/1865ebolaviruscell cyclehigh-content imagingserum starvationaphidicolinnocodazole
collection DOAJ
language English
format Article
sources DOAJ
author Sina Bavari
Rekha G. Panchal
Julie P. Tran
Rajini Mudhasani
Cary Retterer
Jacqueline G. Benko
Krishna P. Kota
spellingShingle Sina Bavari
Rekha G. Panchal
Julie P. Tran
Rajini Mudhasani
Cary Retterer
Jacqueline G. Benko
Krishna P. Kota
High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
Viruses
ebolavirus
cell cycle
high-content imaging
serum starvation
aphidicolin
nocodazole
author_facet Sina Bavari
Rekha G. Panchal
Julie P. Tran
Rajini Mudhasani
Cary Retterer
Jacqueline G. Benko
Krishna P. Kota
author_sort Sina Bavari
title High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
title_short High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
title_full High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
title_fullStr High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
title_full_unstemmed High Content Image Based Analysis Identifies Cell Cycle Inhibitors as Regulators of Ebola Virus Infection
title_sort high content image based analysis identifies cell cycle inhibitors as regulators of ebola virus infection
publisher MDPI AG
series Viruses
issn 1999-4915
publishDate 2012-09-01
description Viruses modulate a number of host biological responses including the cell cycle to favor their replication. In this study, we developed a high-content imaging (HCI) assay to measure DNA content and identify different phases of the cell cycle. We then investigated the potential effects of cell cycle arrest on Ebola virus (EBOV) infection. Cells arrested in G1 phase by serum starvation or G1/S phase using aphidicolin or G2/M phase using nocodazole showed much reduced EBOV infection compared to the untreated control. Release of cells from serum starvation or aphidicolin block resulted in a time-dependent increase in the percentage of EBOV infected cells. The effect of EBOV infection on cell cycle progression was found to be cell-type dependent. Infection of asynchronous MCF-10A cells with EBOV resulted in a reduced number of cells in G2/M phase with concomitant increase of cells in G1 phase. However, these effects were not observed in HeLa or A549 cells. Together, our studies suggest that EBOV requires actively proliferating cells for efficient replication. Furthermore, multiplexing of HCI based assays to detect viral infection, cell cycle status and other phenotypic changes in a single cell population will provide useful information during screening campaigns using siRNA and small molecule therapeutics.
topic ebolavirus
cell cycle
high-content imaging
serum starvation
aphidicolin
nocodazole
url http://www.mdpi.com/1999-4915/4/10/1865
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