Activation of RNase L by Murine Coronavirus in Myeloid Cells Is Dependent on Basal Oas Gene Expression and Independent of Virus-Induced Interferon.
L Dillon BirdwellZachary B ZalingerYize LiPatrick W WrightRuth ElliottKristine M RoseRobert H SilvermanSusan R WeissPublished in: Journal of virology (2016)
The oligoadenylate synthetase (OAS)-RNase L pathway is a potent antiviral activity. Activation of RNase L during murine coronavirus (mouse hepatitis virus [MHV]) infection of myeloid cells correlates with high basal Oas gene expression and is independent of virus-induced interferon secretion. Thus, our data suggest that cells with high basal Oas gene expression levels can activate RNase L and thereby inhibit virus replication early in infection upon exposure to viral double-stranded RNA (dsRNA) before the induction of interferon and prior to transcription of interferon-stimulated antiviral genes. These findings challenge the notion that activation of the OAS-RNase L pathway requires virus to induce type I IFN, which in turn upregulates OAS gene expression, as well as to provide dsRNA to activate OAS. Our data further suggest that myeloid cells may serve as sentinels to restrict viral replication, thus protecting other cell types from infection.
Keyphrases
- gene expression
- induced apoptosis
- dendritic cells
- cell cycle arrest
- sars cov
- dna methylation
- endoplasmic reticulum stress
- bone marrow
- immune response
- cell death
- oxidative stress
- electronic health record
- single cell
- high glucose
- machine learning
- big data
- endothelial cells
- coronavirus disease
- stress induced
- fluorescent probe
- living cells